Synthesis and Structure of Biomimetic Porphyrins: Brian Morgan and David Dolphin

Synthesis and Structure of Biomimetic Porphyrins
Brian Morgan and David Dolphin Department of Chemistry, University of British Columbia, Vancouver, B.C., Canada V6T 1Y6
1. 2. 3. 3. A. 3.B. 3.C. 3. D. 4. 4. A. 4. B. 5. 5. A. 5.B. 5. C 6. 6.A. 6.B. 6.C. 6. D. 7. 8.
Introduction ................................................................................................................................ Porphyrins with Appended Peptides ........................................................................................... CheIatedHemes ......................................................................................................................... Porphyrins HavingCovalently Attached Imidazole or Pyridine Ligands ......................................... Porphyrins Having Covalently Attached Sulfur Ligands................................................................ Porphyrins with Covalently Attached Ouinonc Groups ................................................................. Porphvrins with Covalentlv Attached Interactive Groups .............................................................. "Picket-Fence" Porphyrins and Related Species ........................................................................ "Picket-Fence" Porphyrins............................................................................................................ "Tailed Picket-Fence" Porphyrins ................................................................................................ "Capped" Porphyrins and Related Species.................................................................................. "Capped" Porohvrins ..................................................................................................................... "Pocket" and "Tailed Pocket" Porphyrins ...................................................................................... "Bis-Pocket" Porphyrins ................................................................................................................ Strapped Porphyrins.................................................................................................................... Non-Functionalized Alkyl Straps.................................................................................................... Straps Containing Bulky Blocking Groups ..................................................................................... Straps Containing Interactive Groups............................................................................................ Doubly-StrappedPorphyrins .......................................................................................................... List of Abbreviations.................................................................................................................... References .................................................................................................................................
116 121 127 127 137 142 146 148 148 156 160 160 166 167 169 169 175 184 192 198 199
1. Introduction
Because have ing storage reduction idases in fore A sites. iron each their porphyrin an of iron heir ubiquitousness on as and
4
and
the
variety group,
of are
their
natural
functions, for and P450)5. IX), and the of oxygen b,
heme all c) ,
2
proteins containand oxygen (peroxsite the axial large active of the state, of Thereof
been
investigated porphyrin
multithe
3
and
interdisciplinary electron
levels.
These
proteins,
prosthetic
responsible utilization (cytochrome
transport
(hemoglobin (cytochrome and case ring
myoglobin)l and
transport
(cytochromes
oxidase) , an iron
hydrogen porphyrin essentially be
peroxide oxidation (usually planar
destruction The the nature nitrogens metal. of the of the a (spin
catalases) ', contains occupying of of be fully be
hydrocarbon
active
protoporphyrin coordination by the the of number
four
sites
diversity tenet may to
function
must
dictated is
ligands, the spin and oxidation state of the iron and the nature of he polypeptide chain. basic bioinorganic mimicked understand undertaken chemistry using the in that structure complexes heme protein of and to the function model metal biomolecules simpler which and inorganic the the
Obviously porphyrins state
mechanisms
function,
study
must and much
characteristics steric and has
oxidation
coordination of the
number) on (S 0).
electronic focussed which
effects on upon his the
porphyrin and other ligands are systematically varied. Historically, ism of proteins become (i) (ii) are research binding high spin (S to spin = metalloporphyrins and difficulty = The 2) iron(II) mechanheme is reversible five oxygen coordinate low myoglobin hemoglobin. species, in Oxygen binding
oxygenation behaviour
six-coordinate
reproducing
dominated by two problems: the irreversible oxidation of iron(II) porphyrins on exposure to oxygen, and the difficulty in obtaining well-defined five-coordinate iron porphyrins. Simple the iron(II) porphyrins iron(II) cannot reversibly is the bind oxygen, except by at low of temperature. a second rapidly in
At room temperature, and in the absence of a large excess of a sixth ligand, formation of six-coordinate down, dioxygen to a via species give ferryl immediately -peroxo to give followed bisiron(III) a u.-oxo attack complex. bisiron(III) five-coordinate breaks iron(II) complex This
presumably
intermediate
complex
which the iron has been irreversibly oxidized to the ferric form (Scheme I)8-11.
117
Therefore, the oxygen is irreversible porphyrins must being globin
major site,
role via by
for the to in
the
polypeptide the close
backbone of That
of two
heme heme by
proteins rings fact
is and that
to of the so,
sheath iron(II) body hemocomplex
binding oxidation
preventing ano her
approach is
consequent
[-peroxo reduce to ferric
complex.
irreversible the (the oxidized
oxidation iron(III) Even 3%. This of for
possible an of the in
mechanism the form acid to with
demonstrated functional
provide incapable exists is
enzyme oxygen body and occurs in is
methemoglobin to or the The the under
hemoglobin alternative protonated the the cytoFe11-O2
transport) the aqueous believed occur
iron(II) of conditions
form12. about where
extent
oxidation formation chromes species by
pathway
-peroxo
inhibited, Similar and
involve
proton production
assisted of chain also
formation stabilizes
superoxide13'.
oxidations cytochrome
superoxide,
P45014
oxidase3.
peptide
enclosing
the
porphyrin
in
hydrophobic
pocket
to
which
access
by
protons
is
inhibited.
In addition, recent neutron15 and X-ray diffractionl6 studies have indicated that stabili-
118
zation to
of
the
iron-oxygen bonding of
bond
in the
oxyhemoglobin terminal backbone changes the oxygen is upon
and
oxymyoglobin and the
may
in
part of
be the
due distal a are to is
hydrogen The
between the
atom
imidazole than at has simply the been iron the i.e., In by
histidine (His-E7). influence to to the an be avenue role protein tor more pervasive binding protein in of providing site barrier believed Similarly, provide the oxidation. Conformational of which oxygen on may the active
responsible along in
remarkable residues transfer
cooperativity occur sphere iron
exhibited the the is
hemoglobin17. postulated But it
arrangement
certain electron the
cytochromes.
protein's The second for Eq. 9,
maintaining problem in is =
coordination simple in over
porphyrin preference for the at of
which the
determines the functions of the various heme proteins. major studying example, favoured 10-30 in porphyrins metal N-donor ria the in six-coordination. K2 > K1 For solution at containing 25C)18. strongly benzene coordinating equilib25
0
ligands,
six-coordination (K2/K1
five-coordination,
aprotic solvent
binding the
constants The of one to
of
4
pyridine
-
to
Fe11(TPP) porphyrin high spin (S spin =
have is (S 0) for the
been in = Co", an 2)
estimated
at
K1 spin with is
1.5 (S a =
IO3 1) in on
M-1 state. a
and K2 ~1.9 x IO iron. Addition second field A nate which greater difficult.
M '. The size of K1 and K2 is obviously controlled by the spin state of iron the low In of intermediate five-coordinate species no of stabilization preparing of and mixed for models a to gives the complex which gain adds
four-coordinate ligand form
ligand
six-coordinate
crystal going
stabilization fur her iron the iron
energy19-20.
contrast, this by self is an
gained
from five- to six-coordinate since Co" is low spin in both cases, and K1 > K221). consequence A is difficulty mixed-ligand for thioether form system, a six-coordic in The porphyrins. typical of example is the preparation (His-18) its the with of are cytochrome (Met-80).
coordinated makes control have
imidazole coupled
ligating Strategies
power which
imidazole
tendency
six-coordinate Im-Fe-SR2, range in of
bis(imidazole)
complexes
assembly
ligand
coordination used to
essential oxidation
preparing
heme protein model porphyrins. Numerous approaches been control and coordination model oornhvrin svstems. (i) Excess Ligand: The presence of excess base (imidazole, pyridine) will minimize the
concentration of five-coordinate heme and reduce u-peroxo complex formation.
119
(ii) one
Low is
Temperatures22-'25. where to the reduced studying
Iron(II)-O2 competitive
porphyrin oxygen
complexes reactions as binding
are are K2/K1
stable
at as
low down.
temperAgain
atures
(~-60C),
irreversible
oxidation
slowed increases
temperature
decreases.
(iii) ible Ior
Kinetic oxygen has of to
Measurements: binding Im-Hm-CO, a short preferentially even the exploited
Fast under stability
spectroscopic conditions of with which at a a
me hods where mixture
may
be
used oxida ion and rate
to
observe will occur.
reversTrayA is In
irreversible of the oxygen carbon
imidazole-heme-CO dissociates fast but
complexes
towards carbon The >

(kBO2
oxidation26. monoxide, deoxy IO7 M-'s-1).
solution subjected then
equilibrated laser wi h pulse oxygen
monoxide.
heme
reacts
measurable
IO3 10s, the Im-Hm-O2 complex dissociates and returns to the Im-Hm-CO complex.
Since
kBCO in
is the
the
rate
of and
return
kB
2
before and k^
02
O2 may
is be
added,
kB
CO
may from a
be plot
accurately of l/krelurn
determined
experiment
calculated
vs O2 (pressure). (iv) Metal Substitution: which an Such Ru Replacement are approach In the more is of inert of iron to Co, with oxidation since cobalt28 and Co or possess may ruthenium29 different be leads to with
metalloporphyrins proper ies. Co and
coordination coopera-
applicable
apoproteins
recons ituted exhibits
porphyrins.
case
reconstituted
hemoglobin
tive oxygen binding although to a diminished extent. (v) diethyl The the This to approach a in solid a close be latter attempts support. matrix oxygen covalently approach attached and to oxygen of to In of prevent Wang's polystyrene two was to a prepared the in the was irreversible classic and observed. rigid a silica hemes oxidation a by heme a his with the
Immobilization: the ester matrix porphyrin was not or
anchoring
porphyrin only the
experiment30 but support. gel also
embedded
l-(2-phenylethyl)imidazole. provided and Alternatively, Basolo Reaction removed the iron(II) by support either which
prevented ligand may the the or
approach
hydrophobic colleagues contained Fe (TPP)(B)2 sixth axial However,

11
environment. have undertaken
Reversible
uptake attached and to heating give
3-imidazolylpropyl coordinated base to (pyridine
groups porphyrin
surface31. flowing helium five-coordinate obscured
piperidine) reversible
porphyrin. physisorp-
attempts
observe
binding
tion of oxygen by the silica support.
120
(vi) vented. rin
Steric of The in
encumbrance: two a approach polymer
By
sterically rings closely This of about been
blocking
one the
or u-oxo
both
faces is
of to
the
porphyrin, may the at and the the an sites of of be
close preto the ring steric porphyroom
approach ring
porphyrin most chain. doubts
and
therefore has oxygen
bridge system in of
formation pursued aqueous the or in
mimicking approach the
natural been and in binding
enfold solution
vigorously nature
attempt
prepare
compounds However,
capable
reversible
temperature. In are (i) (ii)
number
active both
reversibility of oxygenation have made this approach less fruitful. contrast, porphyrins by some have group(s) synthesized which to the one ring. faces obstructed covalently bonded The function
hindrance is two-fold: to direct base binding to the open face, ensuring five-coordination, and to allow O2 to bind on the hindered face, steric hindrance preventing u-oxo bridge formation. Five-coordination This ally may has model also be ensured used by in many e.g. these systems to by using a bulky wide axial bases of which cannot bind on the protected face. approach been groups produce variety architecturcrowned, different porphyrins, picket-fence, capped, cyclophane,
strapped, basket-handle, etc., which are discussed below. (vii) allows thioether, likelihood ligand On built-in sixand Chelated one of to Hemes: control etc., to long Covalent the covalent the as for (Eq. attachment of attachment without of the ligand For poor the of a to local addition pyridine, to the ligands large of porphyrin such excess a as of periphery thiolate, and the ligand a of external
extent metal
coordination. the
phenoxide, 15). other As
increases not
concentration
coordination
necessity occur,
(Eq. he 1:1
displacement strong 16), ligands As is
does e.g. long
second
allows formation of six-coordinate mixed ligand systems. hand, imidazole, as this chelation form produces provides mixtures base/porphyrin four-coordinate stoichiometry. dimerization, approach
prevented
five-coordinate
complexes.
In brance fixed energy gained. these
the and
following chelation hat have from
sections as models been the
we for
examine heme in ring. exist
those proteins. order Using of the
porphyrins We to the natural these also create
which review
employ a series with
steric of
encumat on be of will
biomime ic
porphyrins
synthesized porphyrin various reviews
complexes
quinones information can we properties
distances transfer Several models
models, the
important binding
between excellent and their
components which wi h
photosyn hetic ligand systems20,32-37.
apparatus Instead,
discuss
congruency
concentrate here on the strategy and synthetic details of model porphyrin preparations.
121
To
this
end,
the
compounds
have
been
grouped
toge her
more
in
terms
of
structure
than
of function. The reader is directed to reference 56 for a discussion on porphyrin dimers and strati bisporphyrins which are not reviewed here.
2. Porphyrins with Appended Peptides

Perhaps duce tide acids An (Scheme histidyl via the (e.g. early 2). the most to obvious a approach of the to the If synthesis active the of site the of acid the the of by heme protein models is to repropepamino heme various IX by la the IX and
local
environment
heme
covalently fragments
attaching contain sphere who of
various suitable the
fragments
suitable
porphyrin.
peptide
histidine, example After
methionine), of metal his
reproduction was the on to
coordination et
protein may be possible. approach to the into that Lautsch al.38', of coupled histidine-containing imidazole tripeptides was to propionic side-chains length ethyl of side the in mesoporphyrin coordination chain. of peptide
insertion were
porphyrin,
intramolecular chains
possible give
depending attached
Similarly,
histidine-containing sulfide
pep ides
mesoporphyrin Losse
linkages
2(b-d),
a situation similar
to that
cytochrome c.
Miiller39' coupled L-histidine methylester and protohemin 3 with dicyclohexylcar-
122
bodiimide histidine for various ethyl time
in bound di-
N,N-dimethylformamide. to of and to and The a to the the porphyrin imidazole tripeptide protohemin yield reaction in sulfonic methyl attached of the the of Hager41 3 to
However, acid, iron DMF the in
models the length centre. (e.g. in derivatives 6 with of a
indicated of the der Van
that, side Heijden of
with was et
a too
single short coupled and same and the had as 7a-e and prealso
propionic
chain
coordination
al.40',
fragments bispeptidyl mesohemin one or
P-Ala-His; the presence 4a-d
Gly-L-His; 3). At 5 side acids
L-Ala-L-His; the yielded chains such hemins histidine It was
Gly-L-His-Gly-OEt) Warme
triethylamine histidine
chlorocarbonate groups. sulfuric
(Scheme
prepared which ester to the
porphyrins both ei her model quite
containing the
appended complex acid amino both were to a low.
methionine mesohemin been histidine (Scheme methionine paration or
SO3/DMF propionic with or
anhydride,
converted 4). and
into A
anhydride. c
Subsequent
reaction mono7e, also and too
methionine covalently isolation that the and
yielded
disubstituted prepared.
potential
cytochrome products Momenteau the of 9a-c. from was quantities was
containing yields
porphyrin side et arms al.42),
was tedious were
Unfortunately allow of after
recognized intramolecular iron min a
peptide-containing characterized
short
unstrained deuterohe-
coordination. equimolar ester three 9c) was ester) of methyl
have
syn hesized Treatment and
five-coordinate followed by
porphyrin 8 with methyl
coordinating and more The
properties. triethylamine deuterohemin 16% yield
ethylchloroformate desired in
triethylamine, gave, and as a
L-histidine mixture methyl
dihydrochloride compounds separated 9b, and
purification, 6,7-
deuterohemin
6(7)-mono-(histidine deuterohemin mixture of isomers
ester
unreacted obtained
bis(histidine
(Scheme 5). The reduced iron(II) species was capable of binding oxygen reversibly at low
123
124
temperature dimerization
but of
oxidized the
irreversibly species
at
room occurred
temperature. at low
Furthermore,
extensive com-
5-coordinate
temperature
(-60C),
plicating oxygen binding studies.
similar To his of
dimerization stage the 8 three 5or all
was the
observed
for
the yielded
iron(III) model
species systems of which in attached was
at which
room are be in in a
temperature 6-coordinate, tedious. by to 20% the
in or
concentrated solutions. syntheses 6-coordinate la have mixtures prepared solvent after for and species, two with with separation covalently histamine 10 hydrochloric product 2 M could Castro heating of yield of
porphyrin
derivatives mesohemin The hours43).
having
imidazoles, up
deuterohemin
excess
vacuo acid
absence 50% yield
bis-chelated
obtained
purification.
Controlled
hydrolysis
gave
the monochelated hemin 11, again as a mixture of isomers (Scheme 6).
More (obtained prepare and a hemin
recently, from was The series
Molokoedov of yields
et
al.44, ester mixed
have 12 in peptide
used 61%
protohemin yield by 14a-e. using 25%
monobenzyl partial ethyl as Coupling the
ester of
13, to and the
protohemin completed of
dibenzyl by the
hydrolysis),
histidine-containing product
derivatives method 47% to
peptide of
anhydride from
chloroformate length
triethylamine.
decreased
peptide chain increased, the products being obtained as a mixture of the 6- and 7-isomers
125
(Scheme tide 14e This appended derivatives ments, (30-60%) tuted more the
7;
only
the
6-isomers were to 6-
are
shown). to a
The be
reduced for
pentapeptide 35-40 minutes IX with to of of the
14d at
and room 15
hexapeptemperawith two frag-
heme work (a
derivatives was
reported prepare The and or
stable of
ture in chloroform solution in the presence of air. extended of IX in series protohemin condensed methods, mixture that capable chain site c of a derivatives IX various give 6the and having to using is 17, a peptide the fragments45. pentafluoroester 8). Absorption the environment two attempts of of to previously 7-isomers) mixed 15a-i spectra chain the model prepared protohemin monoaminoacyl peptide unsymmetric 7-isomers unsubstiFurtherenhance hemeto to the
mixture protohemin
were as
using
anhydride indicated were bulky the
bisaminoacyl histidine
derivatives peptide
(Scheme
complexes was
residues
pentacoordination. believed c
hydrophobic have been with via His-18
pep ide active The cysteine for of ethyl the
the stability of the 5-coordinate iron(II) derivatives. There peptide be the teau cytochrome the 14 of al.38, chains 17 the active atom et site and the of (Scheme could the c. poor this cysteine to compounds. Sequencing structure sulfide provides with IX of a (16) spectra 17. ligands the various to of he the to obtain of a An to to the the that methyl observed attempt the (TPP) the cytochromes two ligands that reveals heme iron side porphyrin of e.g. residues segment 14-18 bound while
invariant, polypeptide of and
14-Cys-X-X-Cys-His-18. bonds one
imidazole
heme.
Momenprotected
Loock46,
strategy to
similar
Lautsch
attached
pentapeptide iron the then by insertion, metal mimic are covalently
(Cys-Gly-Gly-Cys-His) optical the poor
2,4-a,a'-dib9). bind iron After to would binding of the
romomesoporphyrin centre
appended thioether in was was the
indicated sphere iron. thioether
imidazole
histidine cytochrome
Binding for
methionine, to this overcome case Various a
coordina ion
natural In
However,
thioethers synthetic
made used.
attaching
porphyrin.
deriva ive
porphyrin,
tetraphenylporphyrin
dipeptides
were condensed with the TPP derivative 18 bearing a propenoate ester side chain at a (b-
126
127
pyrrole residue on the

1
position with peptide and
Reaction 19 are and the might
of
a cis-exo in
dipeptide 20 a
containing acid, 10). In
a the
terminal a cis-endo for metal only (R sulfur data be
S-alkvl mixture case, to = a
cysteine of metal two in substituents
cis-meso-tetraphenylporphyrin-3-propenoic cis-endo chain When magnetic residue Zn (Scheme favourable chain was suggested However, disposed
gave
atropisomers, the
conformation that recent a could
binding
porphyrin. cysteine
dipeptide be
Gly-(SR)Cys-OEt EXAFS
Me,
trityl), involving that for long
H-NMR
circular
dichroism occurring. the
bond weak
the the
indicated
substituted
porphyrin,
Zn-sulfur
interaction
and
range, if it occurred at all50.
3. Chelated Hemes
3. A. Porphyrins Having Covalently Attached Imidazole or Pyridine Ligands
Chang imidazole bond51. imidazole would and had On 21 give Traylor either the wi h a the argued too other acid strain-free that or it hand in too of heme-pep ide many was argued 23 models to that XV the achieve 22 side a chains strain-free of by containing the few atoms iron-imidazole of iron heme
condensation followed 11).
l-(3-aminopropyl) insertion "chelated"
chloride
pyrroporphyrin
five-coordinate-system
(Scheme
This
was capable of binding dioxygen in a reversible manner in the solid state or when
128
dissolved -450C, tives the and and of
in only
polystyrene protoring the one 25 and
film.
While
capable at having amide were to a
of
binding or
oxygen
reversibly A
in
solution of For bound
at to 12 The an the or a pre-
irreversible
oxidation ester the then with
occurred or hemes porphyrin coupled excess
room pyridine linkages easily
temperature52. imidazole as was or by by was prepared 24 amine followed then isolated
series covalently in
derivaproto-
pyrro-,
mesoheme
porphyrin mesoheme, 1356. In or 3 The of
through approach was base amine. up
investigated26,53-55. shown partially alcohol one
monochelated
Schemes containing of as
dimethyl
ester primary
hydrolyzed.
purified imidazole
monoacid was
pyridine primary in
using The 30%
pivaloyl pivaloyl 26, yield. 28 reaction
chloride. chloride were mixture The
Alternatively was
commercially equivalent with
available water
protohemin methanol. mixture pared.
treated
base-containing
quenched were
monochelated to
products
chromatography
isomers
dichelated
compounds
similarly
129
The kinetics side
versatility of the the the low 14) at
of O2
the and
chelated CO base,
heme to the
approach these leng h of against a the
has
allowed of
the the
systematic in chelation
study
of
the been
binding and
compounds. and nature
Changes
solvent, arm
porphyrin
chains, Unlike
chelated
have
correlated with changes in the association and dissociation rates of O2 and CO57-58. "chelated-histidine" temperatures, he such binding of the a Traylor to temperatures dimerization IX of the cyanide system argued and design 29, Momenteau42 the used in which of his is and leads vs. underwent any studies26. too binds vice to log dimerizaforms Trayhe allow to tion Ior at presence exhibiting chain While affinity cyanide Y/l-Y (log pyridine polymeric Indeed, For to poorly
(Scheme iron(lll) hemin, titration to the titration centres. Axial ester 32
concentrations side 15). pyridine 29 2.1, to with plot
exploited
system
cooperativity59. short very versa. clean [CN])
protoporphyrin addition of gave base
derivative pyridine greatly pyridine dimer 30. slope
intramolecular
(Scheme increases
Therefore conversion for the this metal
side-chain straight chelation the
protohemin A n Hill =
pyridine-hemin-CN_
line was
of
indicating prepare by two iron rate a
cooperativity symmetric to
between diheme60.
similarly was CO anhydride, with
used
Meso-1,2monomethyl diheme either 33 two
di-(3-pyridyl)ethylenediamine through 16). (Scheme The orientation shifts for published Tabushi heme (22%) stable densation The reaction
1
(31)
coupled followed exhibits of to the the
with
mesoporphyrin give the constants, indicating of
pivaloyl
insertion
environments or a sequential change of environment due to cooperativity. paramagnetic 34 of the for et of and the methyl various al., in have H-NMR were with and heme used the vinyl spectra respect proteins chelated imidazole-cyanide of the of porphyrin ring, these complexes causing shifts for mimic was pyrrole resulted displayed in the the dichelated a fixed values chemical protohemins 35 base studied61. protons. Chelation imidazole maintains different with the
Comparison provided heme
confirmation approach to 37
heme-imidazole of the conas of to
orientations proposed in the natural systems. orientation by groups (Scheme gable cytochrome 17). After 38
c3
62-64
The
"gable-porphyrin" 36 use which with of 39 the
prepared and the
the such
(m-formylphenyl)triphenylporphyrin metal and wi h insertion,
benzaldehyde formation behaviour
dimeric
bridging
ligands
N,N'-diimidazolylmethane porphyrins
g,g'_pyridylmethane bridging ligands
cooperative
the binding of I-MeIm and CO.
130
131
The dimers mate. chlorophyll
H-NMR higher and
analysis converted with 41 42
of it
chlorophyll Denniss to he 18). and by
is and
often
complicated with
by
its he in the
tendency phytyl he imidazole spectra. the A complex
to group
form of
or
aggregates.
Sanders65 anhydride 40
removed resulted of
1
chlorophyll-a
mixed
triethylamine/ethyl
chloroforchelated to the similar formed In
Reaction derivative
l-(3-hydroxypropyl)imidazole (Scheme was used Intramolecular gave Boxer a the 44, well and
binding to
magnesium "chelated
prevented chlorophyll" et al. or
aggregation
resolved Wright of
H-NMR model
when apomyoglobin is reconstituted with chlorophyll derivatives66. Momenteau this ring, to tion series via the the the amide have is ester 45 as gave 47 he in synthesized to linkages derivative a the similar 19). was and series chelated of a by heme of compounds67. Cu(TPP) base attached (3-pyrrole which of cis position Vilsmeier trans tetraphenylporphyrin a Wittig of (70% (TPP) (43)68
(Scheme
formylation
afforded yield and
monoformyl acrylate
elaborated 46. 50
condensation hydrogenathe and corre60%
mixture with
isomers. 48 or
Demetallation, Treatment or 51
saponification acid 49 chloride resulted
propionic
acid
derivative porphyrin
sponding pyridine
l-(3-aminopropyl)imidazole chelated
3-(3-hydroxypropyl)
appropriate
respectively) (Scheme 19). These models were used to study the kinetics of base binding
132
to
4The
and
5-coordinated TPP-acrylic of Cu-TPP using
iron(II) acid acrylic by
TPP69), system acid
and was
also used a 20). nature
to by The of
study Eaton extent the
the et of
transient al.71,72 in the the
oxygenation of
of the
iron(II) carbonmonoxy TPP after photolytic displacement of CO70. same Cu-TPP Treatment acid was chloride 52a wi h nitroxyl resulted nitroxyl, appropriate linkage spinor
labelled
derivatives EPR
52b-f
(Scheme the
metal-nitroxyl
interaction (amide
investigated
varying
ester), and the geometry of the complex (cis or trans). A similar study was carried out on a vanadyl porphyrin73,
133
Collman to the benzaldehyde
et
al.74), position
have of
prepared a (55)
chelated in he hot
TPP ring.
compounds Condensation acetic
where of acid
the a
chain 2% 56. was used
is
attached (53), after with comporphy-
ortho
meso-phenyl
o-nitrobenzaldehyde gave yield
(54)
and of
pyrrole the
glacial
chromatography, with various pounds stannous imidazole 58a-c as
meso-mono-(o-nitrophenyl)triphenylporphyrin mono-o-amino-TPP Collman less and his readily (57) which 21). the colleages merely
Reduction coupled the
chloride chains
produced (Scheme for
substitutes
accessible
"tailed-picket
fence"
rins which are discussed in Sect. 4B. Mashiko et al.75 used the same chelated TPP
134
compounds els for frustrated covalently ligand tem. was These
to by
control c, the
coordination which affinity imidazole of
in of to
mixed iron then
ligand and for
system. imidazole ring a the
Attempts as the rather mixed tail
to axial than
prepare ligands, thioether. amount and
modare By of sys-
cytochrome attaching provided; authors
contain
histidine heme the
methionine
greater the
porphyrin with
stoichiometric lengths
addition prepared
thioether
furnished
six-coordinate
several
complexes
different
various
thioethers. For the Cs tail with tetrahydrothiophene as the thioether, a crystalline iron(II) complex structure determined (Fig. 1). Efforts to were defeated by "head-to-tail" dimerization. (59) (Scheme 22) was obtained and its crystal obtain the corresponding iron(III) complex
Fig. 1. Computer produced perspective of Fe11(C5Im)(TPP)(THT) 59. Adapted from Ref. 75
135
A similar chelated TPP compound 60 was used by Walker to study the effect of axial ligand effect ing a plane of axial orientation ligand ligand on
76
the In (57) to a strain.
H-NMR case In
shifts the a
1
of tail Walker
the was and of and
pyrrole made Benson
protons shorter have to
in used were
iron(III) the monocontainused
(TPP)bis(imidazole)
complexes . bond bound
this to zinc
study
addition, prepare TPP77).
(o-aminophenyl)triphenylporphyrin pyridine
series
derivatives
61a-e
H-NMR
visible
spectroscopy
to study the displacement of the 3-pyridyl ligand by free 3-picoline (Scheme 23).
Condensation porphyrin common 6378). N-I In
of this
57 to of
with the allow
trans-urocanic imidazole was deprotonation yielded
acid to the the
chloride at
(62) the C-4
furnished rather iron binuclear After
the than
chelated the more and 64
case
attached
position addition
imidazolate.
[-imidazolato
insertion complex
deprotonation
Cu(acac)2
(Scheme 24), a poten ial model for he [Cuu2+/Cyta33+] center of cytochrome oxidase.
136
However essentially system.
magnetic
and
EPR
studies the
of
64
indicated coupled
that
the
2+
FeII
3+
and pair (65)
CuII in
centers the to
were natural
non-interacting, et of al.79
unlike used
strongly
[Cuu /Cyta3 ]
Molinaro attach chelated (68) (gave 500C to of ether or (Scheme Goff a
mono-(o-hydroxyphenyl)tritolylporphyrin to the The reacted of to with to may the porphyrin ring via of with did an 65 to not with (71) in the ether and 70 3-(bromoalkyl)pyridine yield. ester condensation was axial a react TTP be bond. reversibly prepare (69), which hydrobromide elaborated base
covalently Reaction of the yield
series
pyridine (65) 67 in
ligands with 40%
linkage. (66) in at
0-hydroxyphenyl-TTP
porphyrin the 25). the The 80C)
furnished 27% low overall
methyl-4-bromobutyrate temperatures affinity. corre(using varying form on imidazoles80. the solvent By in an the effect
porphyrin
butoxy the
cobalt but
derivatives presence
oxygen
enhance forms DMF
oxygen
used
same 72, the
synthetic when chain, the
strategy (65) allowed "tension"
porphyrins dibromoalkane with
appended
Reaction sponding K2CO3 the of length tilting
o-hydroxyphenyl-TTP which, the of alkane gives
imidazole 73 into
Et3N), of or
required
chelated
derivative introduced This was
(Scheme to
26).
molecule have
elongation
iron-imidazole
found
the splitting and shift of the pyrrole resonances in the 1H-NMR spectrum.
137
3.B. Porphyrins Having Covalently Attached Sulfur Ligands

Because cytochrome large heme of the P450 poor have of to affinity usually excess to the of iron(II) of ion. porphyrins solutions to However, the the for of mercaptide porphyrins Traylor81 of has porphyrin in anion, the used models presence the making of of it consisted mercap ide attach metal
concentrations approach for
chelated ligand
covalently
mercaptide without
periphery, excess
available
binding
necessity
external
(Scheme 27). Protohemin chloride monodimethylamide monoacid (74) was coupled to 1-
138
amino-3-mercaptopropane addition CO pound he of 79, dimsyl in CO anion resulted analogous
benzoyl (77) of 80.
ester and the
(75).
After removed was the
reduction the benzoyl
with group, 78. and the
sodium and A
dithionite, addition of give com-
warming mercaptides
formation two complex
carbonmonoxy-mercaptide also of mercaptide
complex as
similar to
containing
masked
prepared
deprotected benzoylthio
Protection
derivative
before reduction of FeIII was necessary because of the reducing ability of mercaptans.
Alternatively resultant
1
protohemin 82 the was CO
was treated
coupled with
with
bis(3-aminopropyl)-disulfide the iron being
(81). reduced
The faster
disulfide of
sodium
dithionite, that the
than the disulfide. Addition of CO then furnished the carbonmonoxy complex 80. H-NMR complexes indicated sulfide underwent intramolecular binding without appreciable dimer formation.
UV/visible band A and (83).
spectroscopy or of
in
DMSO nm) aryl The C6 (57)
solution which was
or
aqueous to
suspension the hyper has or were to after the give iron
showed spectrum
a of
split
Soret
(384/460 series Groh Since
363/446 alkyl and
similar
carbonylated by Collman monochloride obtain, thio the group or the spectra site; iron(II) low-spin
cytochrome P450. "mercaptan-tail" alkyl chain wi h acid to the TrS-K+ thiol. flexible to does lead to to porphyrins may be S-acetyl derivatives porphyrin or hold of the However, been prepared by (Scheme the chain by that in The 28)82. prepared directly treating to the
(oaminophenyl)triphenylporphyrin S-protected was first gave chain were of treatment he alkyl bromoalkyl introduced detritylation indicated spectra, species.
S-tritylthiohexanoyl more 85 difficult and
pentanoic attached either free too
with the was CO
AcS-K+.
Deacetylation insertion, at the
(MeOH/NH3) visible metal
(HgIIZH2S) toluene,
mercaptan planar of
similar
those
square
four-coordinate six-coordinate
introduction
formation
FeII-CO complexes.
To CH3) case quen ly
ensure or the
greater thiol with
rigidity, was sodium
tails
derived 87 as
from were the to
o-mercaptobenzoic attached the to free the 86 or aryl (see
acid 87)
(86; which
= In
or this
(m-mercaptophenyl)acetic potential cleaved
acid
aminoporphyrin. was "mercaptan-tail"
introduced
disulfide give
subseporphy-
borohydride
rins 90 and 91. As in the alkyl case, the aryl iron(II) species did not show five-coordina-
139
140
tion.
Furthermore, on the of
addition nature the
of of
CO the
gave mercaptan to give
mixtures and the the
of
five-
and
six-coordinate suggesting a The
species, tail-off/tailextent of
depending
temperature, was
on equilibrium. Deprotonation mercaptan mercaptide attempted. mercaptide formation depended both on the nature of the base
and for was
of the
the
tail. and a 3.A.
Indeed, complete
for using
most
tails tail
only system anion
incomplete 92, as base. complex
deprotonation to In 93 the
occurred. the of visible (59) as of in
However mercaptide CO this spectrum a model of tailed 60-90% base easy effective
(m-mercaptophenyl)-acetamide gave six-coordinate we c .

75
deprotonation
clean
acetanilide
presence whose
system In for attaching porphyrins (Scheme allowed
iron(II)-mercaptide-CO to the and to the the synthesis of
exhibited a split Soret absorp ion at 450 and 380 nm, typical of cytochrome P450. Sect. the referred ligand with FeII(C5Im)(TPP)(THT) adopted the 94 periphery83. anhydrides or R2SO precluded sulfone > R2S this cytochrome Buckingham 57 iron by Rauchfuss porphyrin sulfoxide, reduction, affinities: imidazole corresponding and ligand or alternative Reaction afforded groups titration > system R2SO2. as strategy the with The an
thioether
(o-amino-
phenyl)triphenylporphyrin 95a-c, 29). the of After following sulfide
containing ordering
thioether, of
insertion pyridine
spectrophotometric
displacement
model for cytochrome c.
141
Smith P450
and
Bisset but A the chains. the followed which to dithiols in
have this
also case
used the
the
chelated substituent leading of
heme is to
approach to ready in the give susceptible the 96
to the
synthesize meso to
potential of an dissuitably 1,6-hexto he the mesorefluxmeso-che98,
model84, at
substituents atom sign with by
were
attached
position of
octalkylporphyrin. placement anediol the functionalized gave of bromide
meso-acetoxymethyl "benzylic" Heating 97 by was 99 ether carbon the with no
nucleophilic with salt 99. 100
introduction a melt 30).
acetoxymethylporphyrin dimer oxidation thiourea afforded to
formation
(Scheme the
Conversion
refluxing the
thiouronium disulfide of of
hydrolysis nately, disulfide phyrins ing
accompanied were
Unfortufrom
attempts complex with
generate yielded
characteristic only the excess of
RSFeII-CO
spectrum treatment
unsuccessful. with a
Alternatively,
acetoxymethylporof in the 21
meso-methylporphyrins. sodium hydride
Treatment provided
acetoxymethyl
octaethylporphyrin containing
l-(3-aminopropyl)imidazole
tetrahydrofuran
suspension
lated imidazole porphyrin 101 (Scheme 30), a potential model for T-state hemoglobin.
The success of the chelated heme approach to model heme proteins is due to its ability to tion control and the coordination covalent binding e.g. of ligands Addition of a metalloporphyrin. to the of the need of For excess chelation base to poorly external can an iron binding the used porphyrin ligand. be ligands local In to the e.g. case in merof their a captide, strongly binding thioether, enhances binding ability. attachment without one imidazole, porphyrin increases concentralower results
pyridine,
equivalent
mixture of four- and six-coordinate species, since K2 > K1 in Eq. 22.
142
However equivalent
covalent of base
attachment which
of can
the bind
base
to
the
porphyrin to give
provides the
stoichiometric five-coordinate
intramolecularly
desired
species, provided dimerization is not significant.
Such model
an
approach
has e.g.
been
followed
by
many
groups cyclophane
to
produce and
an
array
of
different and
porphyrins
picket-fence,
capped,
crowned,
strapped
basket-handle systems.
3.C. Porphyrins with Covalently Attached Quinone Groups

An have approach, similar to interest where earliest 103 of to that prepare as of the chelated with models charge was that heme for model the systems, quinone from Loach a has been transfer adopted event by of state mesodesired Mcintosh of the these electron to an many researchers stimulated porphyrins possible appended groups. excited who Such singlet a systems
primary occurs and with
electron
photosynthesis, One of the
photoinduced such models (102)85. by
transfer of
chlorophyll donors to nearby quinone acceptors. Kong and 105 = prepared he by nature that which chain (p-carboxyphenyl)tritolylporphyrin dime hoxybenzene A et linkage transfer similar who (ester followed Condensation demethylation tritolylporphyrins laser = 3), quinone; flash could suitably furnished prepared and the in the indicated substituted
oxidation have 2, a been 3, 4) studies
porphyrin-quinone pair 104 (Scheme 31). series varied or substituted the EPR (a, b; al.86-87*, both 105 length of and n to the chain (n
amide). from
photolysis adopt
compounds,
especially
conformation flipping of
occurred
porphyrin
subsequent
extended conformation could then prevent recombination and lead to a long-lived radical
143
ion lar of
pair.
Wang rings
et with have
al.88', to an
prepared the appended
series
of
porphyrins by were lipid
106,107 amide also
having
either (Scheme and
one 32). both
or
two Simi-
quinone
attached
porphyrin
periphery group bilayer join and into to
linkages prepared,
porphyrins compound The use
carotenoid
classes in can vary.
been or the
incorporated ester the linkages
membranes. and the
Photoconductivity quinone moieties can of quinone later
such membranes was enhanced relative to simple membranes89. of amide as to more the porphyrin of lead to complications solutions use of both separation of to orientation two centers and and
Possible (i) the
problems spacers and
porphyrin-quinone separate strapped ion the
orientation porphyrin are
prolonging (models in the onto
the change-separated species have included: rigid strapped the employing (ii) attempts capped, to doubly quinones pair by described other
appropriate sections); stabilize transient radical introducing groups the porphyrin.
144
Tabushi chloride in observed extended tion TPPBQ the tively). of (108), which
et the but
al. which, no the 110 111a.
have after
reacted selective was
mono-o-amino hydrolysis is proposed. fixed in and reaction TPPAO and Hlc and fixed. The
TPP oxida ion, Efficient
57
with
2,5-diacetoxybenzoyl 109 distance (Scheme quenching has 34)91. the 18% 33) was been Reacproduct of rate respecThe
furnished
porphyrin-quinone mechanism relative (25%). TPPNO
distance
fluorescence llla-c yielded prepared (15% 10.5 and for
porphyrin-quinone pyrrole with were at 10,
and
orientations Diels-Alder Illb with distances charge and
compounds
(Scheme gave by and 11
2-anthraldehyde,
benzaldehyde
meso-(2-anthracenyl) condensation
triphenylporphyrin (40%) The corresponding for
benzoquinone
2-aldehyde
pyrrole were
benzaldehyde and
porphyrin-quinone photoinduced
estimated
A.
constants
separation
recombination
these
compounds
have been reported92. The condensation of a linear tetrapyrrole 112 and an aldehyde to
145
form The
mesosubstituted (Scheme 35) bicyclooctane
porphyrins with yields units
was
used flexibility
to and base
prepare only and
another distance rotational
series (6, 10 freedom
of and is
compounds 14 an with the ylide free order may
113-115 Preliminary A systems substituted porphyrins showed in which
increasing of the of which the double The rate
porphyrin-quinone free
)93.
eliminate
allowed. increthe meso11794). base to thus systems prepared96
fluorescence
zinc
porphyrins was
indicate observed of the in In was and
mental effect of distance on photochemical electron transfer93'. similar shown incremental in Scheme 116 of 119a, effect 36 (as the b. porphyrin-quinone were nickel bonds of on the a prepared complex) and the then separa ion by Wittig the with condensation phosphorus furnished transfer the 120 chain95.
porphyrin reduction and inverse a the pair 118
Deme hylation, an
oxidation electron of
photoinduced
such
exponential electron quinone of
dependence transfer rings
length
demonstrate
multistep
bis-quinone redox
porphyrin potential
provide
gradient
stabilize charge separation. Comparison with the mono-quinone etioporphyrin 119a
146
showed the is for much the
approximately time longer was than of
exponential much for 120 to A was
decay for
of 120.
the he
charge
transfer of Moore
state the et both the
in
both
cases, in in and to
but 119b 120 a the
decay
longer
Similarly
photoinduced
charge second al.97, a was
transfer quinone used quinone
demonstrating prepare a by
importance states. separated
generation group
long-lived
charge-separated system charge electron
5,15-bis(4since
aminophenyl)-bistolylporphyrin carotenoid charge 121. recombination
incorporating transfer from
photodriven inhibited
complex
observed
porphyrin cation radical, to give a long-lived (us scale) C+ -P-Q - species.
carotenoid
3.D. Porphyrins with Covalently Attached Interactive Groups

A than and tion variable number of o her have 122. the "tailed" prepared Both porphyrins a series and the have of been or derivatives EPR terminal prepared which a contain groups other Maiya chain the of tail to interacpotential Krishnan98 length between Similarly a cyclodextrin 123 did While ligands. Using mono-(mand p-hydroxyphenyl)triphenylporphyrin, containing data group, was guest phenoxyglycol intramolecular that suggesting covalently oxygen in inclusion indicated
fluorescence ring
porphyrin
phenoxy (65) a
existed in a folded-over conformation. mono-(o-hydroxyphenyl)triphenylporphyrin unit, not in the display hope the of preparing desired attached carrying the water-soluble model99.
properties,
cyclodextrin
moiety appears to induce novel conforma ional changes in aqueous solutions.
147
Other
cyclodextrin included of a Fe11
capped in an
hemes
have
been which
prepared101 formed oxygen porphyrin could a
using
1-substituted
2-mecomplex exploited Covalent
thylimidazoles with protoheme. The by the Lown 124a-c series and ability of
a-cyclodextrin to generate to
pentacoordinated has deliver rise an to been the DNA A a
porphyrins prepare DNA where
reactive an of iron
radicals might give with
several DNA and of
groups
to
systems reactive a of
with
potential species
antitumour
properties.
attachment
suitable surface
intercalator
heme
to
helical
oxygen series the
scission. acridine similar spermine
Joshua101 mimic in
have the a
prepared properties 125,
deuterohemins from
attached
which
glycopeptide is bound to
antibiotic the
bleomycin. via
compounds which
126,
derived
mono-p-aminophenyl)-tritotyIporphyrin porphyrin
protohemin,
suitable
intercalator
chain, has also been prepared which exhibits oxygen-dependent DNA cleaving ability102.
148
4. "Picket-Fence" Porphyrins and Related Species

4.A. "Picket-Fence" Porphyrins
Perhaps porphyrin (i) due the of to most successful Steric of the heme protein about adopt to the a active metal site site models of in is these which the "picket-fence" TPP mesoat the and, Collman. steric rings encumbrance the TPP will substituted the four
molecules depends on two factors: repulsion, are conformation the porphyrin phenyl phenyl (ii) for essentially perpendicular ring; substituents separation the four
orr/io-positions of the phenyl rings will lie above and below the porphyrin plane, and TPP molecules on the that containing bulk of mono-ortho-substituted the of the thereby subs ituent, a same could dioxygen could groups and four rings, of depending Collman four could of bered stable "protected not and since excess interconversion iron(II) the the metal possible having give face a but
atropisomers may be achieved. reasoned groups pocket". ligand. a the of the (4a, was 3ab the syn hesis on e.g. much substituted side bind of to tetraphenylporphyrin ring the in be would open the sterically oxidation on even not pivalamido located porphyrin
Ligands the The bulky
imidazole, smaller complex
penetrate
pocket,
ensuring form. should
five-coordination would This
presence encumbe through (53) in four moving was
molecule
six-coordinate
oxygenated
complex
should
pivalamido (55)
prevent of
irreversible
close approach of two porphyrins and formation of a u-peroxo complex. Condensation acetic chloride atropisomers of which acid to gave pyrrole equivalents 128 by o-nitrobenzaldehyde was reduced 37)103,104. the the of by The slowest meso-tetra(o-nitrophenyl)porphyrin 2a2b) were separated 129. which stannous
meso-tetra(o-aminophenyl)porphyrin desired aaaa isomer
(Scheme
chromatography,
Interconversion
atropisomers
sufficiently slow at room temperature to afford clean separation. Refluxing the unwanted
149
products further gave frozen zation the by of
in
toluene of
for he
20 aacta
min
effected
reequilibration of the on
to amino
the in
statistical with the which with
mixture pivaloyl and
allowing chloride is by isomeri-
isolation the these
isomer.
Reaction
groups
"picket-fence" bulky
porphyrin substituents.
II
a,a,a,a-H2(TpivPP) Several been studies made105-107'.
130, the
configuration followed
physical
properties FeBr2,
atropisomers
have
Treatment
reduction with Cr(acac)2 gave Fe (a,a,a,a,-TpivPP) 131.
Although "picket-fence" compounds pyridine, reversible amounts
addi ion side was was
of it
strong was less (B than
field that Im, in
ligands that on the
gave the
low
spin constant A All 25
six-coordinate of the of series of C,
complexes, on the six-coordinate l,2-Me2Im, showed appreciable (N-RIm)(O2)
FeB2(a,a,a,a-TpivPP),
suspected =
binding "open" l-n-Bulm, solution
base
side.
prepared binding
l-Melm, benzene the
l-trityllm, at
4-t-BuIm, these without
piperidine, oxygen of
tetrahydrothiophene, behaviour Indeed,
tetrahydrofuran)104. oxygen
decomposi ion.
complexes,
Fe(TpivPP)
were stable for long periods (ty2 2-3 months) in solution provided 2-4 equivalents of axial
150
base talline
were
present
to
protect 132a
the could (Fig.
unshielded be 2)104108,
face.
Furthermore, The
analytically crystal EtOH
pure, (Fig.
crysof 3)
dioxygen
complexes
obtained104.
structures
Fen(TpivPP)(I-MeIm)(O2)
Fe"(TpivPP)(2-MeIm)
and its dioxygen adduct109 (Fig. 4) have been determined. Further structural information
Fig. 2. Perspective view of Fen(TpivPP)(I-MeIm)O2 (132a). Adapted from Ref. 108
151
Fig. 4. Perspective view of Fe(02)(TpivPP)(2-MeIm). The dioxygen and imidazole are disordered. The disorder has been idealized and only one concentration is shown in this figure, which is adapted from Ref. 109
152
was also
obtained been Binding
by
I.R108,110,111 The reversible Reviews
and on
Mossbauer of oxygen binding
spectroscopy to to cobalt picket side
and fence, of heme under the
magnetic of and
susceptibility TpivPP has systems prevented However, give O2 (B the and Similar = that
measurements82'108*.
binding
oxygen
complexes
studied112. of of a
related
have also appeared32-37 113-115). second oxygen base binding could on to could be the the be "picket-fence" porphyrin solu ion. to between cycles116. was region the to of Fe(TpivPP)B it regions of of determination crystals vacuum reversible 2-MeIm, solid tive on state binding of five-coordinate five-coordinate deoxygenated oxidation solid and a are in the Y vs. an re-oxygenated. by Y/l in
FeII(TpivPP)(I-MeIm)(O2) species no From binding and iron rationalized as the of the high which was the for low this and observable Hill
vacuum many of
This over log samples
cycling
produced l,2-Me2Im). oxygen (at
irreversible plot (log two terms bound the
oxygenation
demonstrated these O2 in its in
P0z) two
concluded
compounds of solid strain
showed
non-cooperacooperative dimensions ring. As molecular conformadeoxy condenchlorides. H2(TTOSPP) p-toluenesulthe ferto exposure and been
pressures)
intermediate of the this towards
binding. increasing
Collman numbers in
shrinking move
molecules' porphyrin in a change induce the
oxygenation
imidazole
molecules induces solid which
oxygenated the crystallite affinity been with
dimensions tional
presumably
sufficient
change
enhances TPP
oxygen have 129
remaining by the
sites. This behaviour is reminiscent of the cooperative oxygen binding of hemoglobin. Various sation Collman (136), fonyl rous oxygen directed quent The yielded be CH3I, para by of et other al. reaction 134 of
0
sterically have of
hindered
derivatives the with 38). the of with a to
prepared bulky (135) 133
meso-a,a,a,a-tetra(o-aminophenyl)porphyrin also prepared (129) (Scheme to H2(TAmPP)
acid and and on were
compounds, iso-phthaloyl Despite only acidic of TPP
H2(TphthPP) dichloride bulky protons the
chloride complexes at heme 25 into
respectively both This cavity, A was
"picket-fence", which
compounds attributed similar allowing
exhibited protona ion series (129) as
irreversible amide the
oxidation
presumably consesyn he-
the
coordinated
dioxygen have chloride hen The potentials, ligand of
oxidation104*. of
derivatives
137a-g
sized under identical conditions by Bogatskii et al.117-118. reaction the by by o-H2(TAmPP) TPP excess isonicotinic of groups the and used For water 39). reduction as were hydrochloride which could with tetra-isonicotinamide anion statistical yield mixture atropisomers soluble
separated followed and
chromatography.
The
isonicotinamide (138)
methylated
exchange, were also have
tetrakis-(N-methylcorresponding basicity systems and by
isonicotinamidophenyl)porphyrin-tetracation meta deriva ives TPP
(Scheme
prepared been
reactivity with metal ions of the isomers were compared119. Ort/iosubstituted choosing suitable derivatives on the binuclear substituents phenyl rings. example, treatment a,a,a,a-
H2(TAmPP) 129 with maleic anhydride gave the tetrakis(o-maleamoylphenyl)porphyrin
153
(139) insertion the
in at copper
90% a by
yield rate the
(Scheme much faster carboxylates capable the
40). than holds of
In
aqueous for the metal iron of
DMF ion and in
this a
porphyrin Rapid position have
undergoes favourable for
copper of rapid as 141
unsubstituted
porphyrins.
complexation
intramolecular transfer to the porphyrin nucleus120'. Binuclear synthetic porphyrins for binding site copper been One inves igated model models iron/copper cytochrome oxidase. such
consists of a tetraphenylporphyrin ring with a covalently attached tetrapyridine ligand
154
system, (140) ring and claim tion tions and
obtained (Scheme copper the
by 41)121.
treating The to of
a,a,a,a-H2(TAmPP) metal four for the compound the the
(129) with
with iron In
excess inserted was contrast,
nicotinic into Elliott cause Ru" the and
anhydride porphyrin the and to EPR Krebs the condimetals
mixed
coordinated conditions
nicotinamide metal insertion these divalent into
groups into place and
prepared, complex more
magnetic that of to the be
susceptibility nicotinamide
complex Instead, of
examined12'. authors
necessary groups123. locks the
this have
isomeriza-
coordinated first-row
nicotinamide
groups, used
which for
"pickets"
allowing
forcing transition
introduction
trivalent
into the porphyrin ring, without fear of isomerization.
155
Iron oxidants have chiral strate
porphyrin is believed the the
catalysis to catalytic porphyrins iron-oxo with group was The was (142)
of
epoxidation via a
and
hydroxyla ion of olefins of
using using were
iodosylarenes and of by was group cavity acid iron 20-50% 42). suitably
as
proceed to
reac ive the The chiral
iron-oxo
intermediate.
Groves
Meyens suban
attempted olefin to
asymmetric control species124. an as in the the
epoxidation chiral active
substituted the With reacting formed was about (144) insertion. were
"picket-fence"
stereochemistry porphyrins acid of the various Instead and by
approach prepared 143a with chiral and of (Scheme
a,b,a,b-H2(TAraPP) in very chosen the was This high little as yield an
optically
chloride
(R)-2-phenylpropanamido (95%). selectivity core. with 143b
appendage 9-31%). a large of followed
porphyrin olefins the rigid
However, which
epoxidation form
iodosylbenzene
obtained could diacid -H2(TAmPP) more
(%ee, chloride (142),
binaphthyl
appendage
relatively
porphyrin reacted catalyst
l,l'-binaphthyl-2,2'-dicarboxylic methanolysis excesses enantiomeric
a,b,a,b
efficient
and
observed for variously substituted styrenes and aliphatic olefins.
156
More ence ence of of
recently HCl acid to its
Tabushi as
et a and
al.125 cytochrome slow pickets However, phenyl
have P450
used
oxygenated on Under ferric of
Felll(TpivPP)Cl conditions followed has
in in by been are
the he
prespresis
and
H2-Colloidal
platinum
supported mimic. of the
poly(vinylpyrrolidone) such complex the that ring this
chlorides
cyclohexene
converted A with
epoxide 145 =
reduction on
formation prepared substituted will be a
of the dioxygen ferrous complex completes the catalytic cycle. porphyrin 43; R' the bis-ortho bearing CH3)126. both so it faces is (Scheme only two opposite unlikely meso-positions
substituted
rings
compound
successful oxygen binding model.
4.B. "Tailed Picket-Fence" Porphyrins

While solid base prevent is complex the state, direct such oxygenation studies in To to in the control of five-coordinate were not of presence FeII excess on Collman "picket-fence" since sterically the et "open" al., the was observable base. prevent the in the not solution complete possible "picket-fence" face and could
six-coordination necessary formation.)
unhindered adopted
(Excess (-oxo "chelated
ensure
coordination
coordination,
heme" approach. Dispensing with external ligand, the base was covalently attached to
the
ortho-phenyl
position to
of the
TPP, porphyrin (129) 146 free to were
and
so
constrained The other
into three of
position
promoting rings gave a and carry he solu(3 aor vary-
intramolecular Treating "3-picket" tion for 2
binding
metal. with (35%) 3.2
meso-phenyl chloride in of (The by the Using
the "pickets" necessary to prevent irreversible oxidation. a,a,a,a-H2(TAmPP) a-aminophenylporphyrin h equilibrated 146, be an 147 the which was equivalent 44). to of a group by yield 149. the pivaloyl Refluxing 1:1 the mixture b-product.) 147 iron(II) (due 25 to in insertion (Scheme benzene unwanted amide of chains using "tail C) a
aminophenyl separated the to and of increase 148 spectra but on were had
atropisomers isomer urea ing FeBr2 spin to a (S could linkages leng h gave =
chromatography.
re-equilibrated imidazole the
attached yields
he
P-aminoporphyrin Direct the the metal five-coordinate
to e.g. 2)
yield nearly iron(II) (S
porphyrins
1
anhydrous picket-fence" high due peaks
quantitative H-NMR 0) not formulation, = but
porphyrins,
15174.
confirmed decreasing observed, observed
proposed
five-coordinate
temperature presumably such
diamaenetic
complex Travlor.
dimerization the chelated
Drocess.
(Momenteau.
dimerization
heme systems.)
Addition the peak plexes, A pyridine The and Sect. fence" thioether aryl
of
oxygen spectra for the
to of
solutions a "pickets" the
of
the
high that of
spin the the
five-coordinate for the a may be
iron(II) ordered
compounds species in which 151. these is
gave The com-
expected pattern
diamagnetic suggests open side
compound
oxygenated suggestion has urea been
oxygen pocket,
presumably similar
towards of
awaiting with and of of a CO alkyl in the
confirmation by X-ray crystallography. series "tailed to picket-fence" the porphyrin porphyrins periphery 57 P450 been the 150 via to synthesized O2 covalently use 3.B. A of attached linkages127. a by
binding to both series of porphyrins has been carried outl27_l29. meso-(0-aminophenyl)triphenylporphyrin porphyrins series of as 147 45)82. prepared cytochrome has give A and similar is to similar 154 also compounds prepare has series acylation "tailed an reversibly with of mercaptan-tail models alkyl been described
prepared 155
tripivalamide-|3-aminophenylporphyrin porphyrins chain has (Scheme been
mercaptan capable
picketappended binding
compound reportedly
dioxygen74.
5. "Capped" Porphyrins and Related Species

5.A. "Capped" Porphyrins
The rins direct was a condensation exploited by benzene tight On that the which probably "cap" to porphyrin. ring the other should to a result give Unlike of was aromatic and aldehydes co-workers to to attached bases on the smaller a physical a low and all pyrrole four to form tetraphenylporphyIn the these mesobe fit It of Baldwin prepare "capped" porphyrins.
molecules was nate under was linkages attached the rin ring
covalently of the
or//io-positions
phenyl rings, enclosing a volume of space above one face of the porphyrin ring. If the cap sufficiently on the species. the recognized would to the binding face; hand, (e.g. open alkylimidazoles, face to would [x-oxo a the molecule with pyridine) result would in be by a should able four units to the to prevented enclosed binding five-coordi-
dioxygen barrier ring was
cap,
provide in the
complex porphyrin with necessary of
formation.
attempts
condense very
benzene yields. which
ester were give is
Instead
tetraaldehyde
condensed
pyrrole
"capped"
"picket-fence"
porphyrin,
cyclization
porphy-
is the last step of the
synthesis, so chromatographic separation of
atropisomers
not required.
The with 159.
required of
tetraaldehyde to the yield
156 158,
was with
prepared by pyrrole in
by
alkylation refluxing
of with
salicylaldehyde pyromellitoyl acid yielded
(157) chloride the
bromoethanol Reaction
followed
condensation
tetraaldehyde
propionic
"capped" porphyrin 160 after chromatographic purification (Scheme 46) (Fig. 5)130,131.
Fig. 5. Two perspective views of the "capped" porphyrin 160 as the free base. Adapted from Ref. 140
The
same
reaction
sequence or
using
2-(3-hydroxypropoxy)benzaldehyde porphyrin the on 161 extra he in which there
yielded is an
the extra to
corremethythe
sponding was larger
"homologous" lower To (5%),
"C3-capped" probably steric
lene group in each link of the cap131. In the latter case the yield of the cycliza ion reaction much cap. reflecting hindrance entropy uncapped factors face required a form provide "naphthyl-C2-capped"
porphyrin 165 was similarly prepared (Scheme 47) from 159 and 162 via 163 and 164131.
Inser ion crystalline containing
of
iron axial
into base
the the
"C2-capped" spin iron(II) five-coordinate
porphyrin, porphyrin heme
followed 166 was formed
by
reduction, 46). was In
gave capable
a of
four-coordinate excess
high
(Scheme
solutions
which
reversible dioxygen binding at 25 0C The stability of the dioxygen adduct depended on
the axial that side
nature base, they of
and the were a
concentration Unlike larger small, the size e g., of
of the
the
axial
base
and 166
the which
position could of two bases iron,
of only axial
the
equilibria a
in
Scheme
48130.
"C2-capped" propylamine. could binding was
porphyrin For still
bind bases, as a
single provided it the
"C3-Cap" weakly
permitted coordinate reported
binding size to to
intermediate
such
l-Melm, through
appeared
that the
second
base
the
probably
cap.
Oxygen
occur,
giving
pseudo-seven-
coordinate complex132-134).
The been natural
O2,
CO -
and . It and
NO
affinities found
of
series O2
of e.g., >
FeII the
and were Fe"
CoII much
capped lower (167)
porphyrins than of > those
have of >
studied
131 137,l38
was other >
that
affinities
porphyrins
synthetic
models (160)
complexes
H2(TAP)
H2(NapC2-Cap)
(165)
H2(C2-Cap)
H2(C2-CapNO2)
H2(C3-Cap)
(161). In contrast CO bound more quickly than O2, and the rate of binding was indepen-
Fig. 6. Perspective view OfFe111Cl(C2-Cap). Adapted from Ref. 141
dent
of
the in
cap terms
size of a (Fig.
and steric too 5)140
comparable effect small in of to and exist
to the
unhindered cap. (Fig. the
model the 6)14
porphyrins139. crystal or that O2, a system However, of the
This of the
was both phenyl be bent
ra ionalized H2(C2-Cap) cap-porphyrin more Fe-O-O
Although either
structures
(160)
FeIIICl(C2-Cap) solution. against by a a
indicated CO Fe-C-O effect. effect
separation version under might
was must cap be
accommodate That "central"
considerably could the
expanded system
linear steric steric
accommodated chain linkages.
the
argued
destabilized
"peripheral"
methylene
Studies142,143 used to deduce > NapC2-Cap
of
the the >
paramagnetic C3-Cap,
shifts which
in
the The
H-NMR the
of
CoIICap size was
porphyrins in the affinity a
were order of mod-
cap-porphyrin
separation.
relative with been is
cavity
C2-Cap the
correlates has
relative to
oxygen prepare to two
the iron(II) "capped" porphyrins. Recently144 ified "capped porphyrin porphyrin" in which approach a extended "C2-capped" pyridine covalently bound opposite
meso-aromatic rings of the parent "C2-capped" porphyrin, forming some kind of "strap"
(see lowed
Chap. by
6) were
over
the For
porphyrin by solubility with
face reasons the
opposite of it a was
to
the
"cap". to
Bis-amino with benzylate diacid
"C2-capped" pyrrole the folamino Both
porphyrins functions
prepared
condensation
dinitro-tetraaldehyde necessary 3,5 pyridine
reduction. before
condensation
appropriate
compound.
of the corresponding iron(II) C2-Capped strapped porphyrins 168a, b exhibit reversible
oxygen of not low that the
binding
in
toluene (the complex
solution 168a the
at is strap for
room several and
temperature 168b cap has a months).
and t of
show several
good days
stability while
to that does a
autoxidation result affinity of
reactions in of of of a a
C5-Strapped
complex
C4-Strapped -oxo the the
Furthermore, dimer of of 4 locks the binding on
decomposition formation.
complex,
preventing Comparison has a a factor by of
Although values shows
kinetic study has not been made, it appears that the stability to autoxidation is due to the iron(II) strap complexes complex decreases interactions. configuration The to the the The dioxygen. (which O2 affinity also the O2 for P affinity) the the metal of with that iron(II) C2-Capped (166) low
introduction combination complex porphyrin metal more tic in offers steric
C5-Strapped unoxygenated towards to the the
complex 168b, and by a factor of 40 for the C4-Strapped complex 168a. This is due to a steric domed presence resists the the of the and the the cap of the metal porphyrin which the movement strap of
upon
oxygenation. further may
presence
pyridine the This
resistance motion of
movement
oxygenation. and
Furtherbe
interaction
occur
between pyridine
pyridine
side-chains
meyo-aromawould
rings
preven ing
towards
center.
more severe for the shorter C4-Strap, resulting in lower dioxygen affinity.
5.B. "Pocket" and "Tailed Pocket" Porphyrins

To rin is the ide prepare et to approach used to can only by only of a al. to system have which used a discriminates a series of at against of one Fe-O-O bending (129) under The of was with high volume the "pocket" leaving the the face unit binding of CO and As relative the but in above, Oxygen open of he than side. linear one 49). afforded was a may to that of O2, ring it is within monoxunit of Collman combina ion "picket-fence" of an and/or the open toward tilting "capped" this porphy-
prepare steric three be
porphyrins145.l46.
benzene case bind Fe-C-O equivalent the
provide
encumbrance of the bent by
porphyrin, side. the
linked
raera-phenyl accommodated
groups,
pocket
orientation
Carbon
leading to decreased CO affinity. Treatment pivaloyl with choice a of porphyrins irreversible a,a,a,a-H2(TAmPP) formed tris-acid in good A chloride the yield and similar chloride the 170 sligh ly dilution of single the to more 169 chloride benzene 171 acid "mono-picket" (>60%). porphyrin (Scheme conditions pocket picket Condensation pocket by the against
dictated protection the
presence strategy
provided prepare
oxidation.
employed
"tailed-pocket"
porphyrins 172. However, in these compounds, the remaining ortho-ammo group is used
to attach the base, leaving no protection on the open face of the pocket. In contrast to the "tailed For the Piv) tration nant were similar size picket-fence" the of the ranges species. iron(II) the from porphyrins, "pocket" 171a be O2 While a model these porphyrins, five size complexes the undergo rapid state spectral in the of data oxida ion the iron of was to the -oxo on complex145. coordination and MCD even showed the both in CO Since depended that excess he the effects to the pocket. and and the reduced Visible remained large CO O2 CO the absorption showed Fen(Pocbase. concendomi"pocket" were steric porphyrins
derived
coordinate pockets within of for which
presence iron(II)
Although
medium could The
increasing and were and was
six-coordination, "picket-fence" similar, solvent attributed
determined
five-coordinate "pocket" systems electronic affinity
binding affinities affinity.
compared147. showed he two in
porphyrins
systems,
reduction
hindrance of the cap which distorted the Fe-C-O unit from linearity.
5.C. Bis-Pocket" Porphyrins

Eventual occurs this, steric the irreversible because bulk for but the (where steric the ring. would (P2-) oxidation TPP of both is the have protected s ill the be to dianion by "picket-fence" only on one been pocket and side be by of of By axial two have the the the "capped" molecule. on metal prepared both and the choosing bases porphyrins To he avoid correct sides of thus hemes or trisubdiatomic encumbrance present a
octa-ort/io-substituted ortho The porphyrin
complexes could
prepared. may
substituents pockets a barrier the
formed
penetrated approach Vaska of and
molecules stabilizing FeII(P)
form is
close of
centres,
oxygenated
porphyrin.
Amundsen
tetrakis[2,4,6-tris(methoxy)phenyl]porphyrin appropriate
tetrakis[2,4,6-tris(ethoxy)phenyl]porphyrin)
condensation
stituted benzaldehyde with pyrrole148. Balch has shown by 1H-NMR that although the
or ho-methoxy ature role prepared in reduction sterically which natural was he However, binding site. Covalent to by 175 prepare Lindsey was by gave
substituents to Suslick the form and propionic base, of
prevent Fox149, acid
-oxo and who
complex
formation, A
oxidation more in 1%
at
room
temperwas pyrand the

0
proceeds refluxing
FeIII(P)OH to
Fe111(P)Cl11. condensed the species 173 a
hindered yield. yield.
complex with of 30 and of be Metallation
2,4,6-triphenylbenzaldehyde in in to 80%
obtain iron(II)
porphyrin gave to
four-coordinate completely affinity is
Addition iron(II) at
hindered capable
1,2-dimethylimidazole, reversible very which to low was the a a
five-coordinate non-polar model the of other
complex C the the used the
oxygenation compared attributed four
solvents
oxygen an
complexes nature also was
systems,
observation of a
non-polar TPP an may
attachment porphyrin and
group to rings
orr/iopositions structure. Such 10 was
complexes the two
having was of and high the
rigid
approach system The of yield in
adopted
Mauzerall150 by The at
prepare
cofacial to 174, of for
porphyrin-quinone be
separation H2(TAmPP) reaction porphyrin bases (Scheme porphyrin gated and mated151.
between prepared (129). were after
estimated the yield desired groups
where
quinone-tetraaldehyde with of the of a,a,a,abase Schiff yield zinc estiinvesti"capped" the the was the Schiff
alkoxylation reversibility for the room yielded of The the for
fluoranil
which the
then nature 85%
reacted
intramolecular reaction; h. and 24
responsible stirring NaBH3CN Acetylation 177. rate
temperature amino electron
Subsequent metal of
reduction 176
with 50).
porphyrin-quinone properties this porphyrin
80-95% were
insertion to
furnished quinone
quinone he
photochemical
compound
constant
transfer
from
6. Strapped Porphyrins
The which formed strapped some porphyrin group is thus The class usual allowing pagoda, of heme linked synthetic great protein to two strategy versatility models corners has in he The is will to embraces (usually to types tie of all the those strap may face compounds opposite) to be of an made singlythe of in a covalently diagonally
porphyrin
macrocycle. porphyrin, crowned,
been
already (e.g. or
structures
cyclophane, (i) (ii) (iii) Simple Straps
basket-handle, alkyl chains
etc.). role
porphyrins span one
doubly-strapped and may be classified according to the nature of the chain: non-functionalized incorporating straps the or to whose porphyrin, discouraging -oxo bridging and providing a more hydrophobic environment. some which metal at form bulky group which some provide more steric of be encumbrance to or than a simple alkyl chain. Functionalized interacting with five-coordina ion incorporate the group These capable may ligand binding used to L-M-L', porphyrin core. mixed maintain where
six-coordinate
systems
one ligand binds poorly to the metal.
6.A. Non-Functionalized Alkyl Straps

A number of research groups have reported the synthesis of simple strapped porphyrins. Ogoshi et al.152-154'condensed long-chain diamines with a difunctional etio-type porphy-
rin
178
in 51).
the On
presence the of
of
isobutyl 179 of (n
chloroformate = 6-10, axial to absorption
and 12) in
triethylamine 20-30% he it
under after was to was
high claimed the II side or 184
dilu ion that,
to for por-
obtain short phyrins used yield ester yield. to
the straps, at the
strapped binding iron(II) 15 same

0
porphyrins basis a
yield strap
chromatography inhibited, ferrous et (180) in chains in the giving al.135' with 25% by good ferrous oxidation strapped P450 by
(Scheme
visible bulky
spectroscopy under oxygen the -oxo of the
second in
ligand of
five-coordinate
species. resulted
Attempts rapid high the
observe
binding
forma ion bis-acid to of dilution by
complex.
Battersby 182
strategy, (181) 52).
reacting under
chloride give the
mesoporphyrin porphyrin coupling 183, to an as carboxyl
1,12-aminododecane (Scheme or amide gave the THF in ferric 185a to 185a has natural steric were benzene.
bridged oxidative
Alternatively, the strap or ester-, can aqueous Chang 53). the In cases or
elaboration
porphyrin
formation,
followed easily acetone and this the into
intramolecular strapped
0
Dieckmann
condensation complexes the porphyrin model iodosyl ligand models by the increased A Unlike of the
amide-linked move at
156
porphyrins only rapid
Because
sideways 20 have the itself A 5-7 the Raman the by C also system
attempts prepared was as series of
oxygenate
showed
irreversible amide-linked a
state. (Scheme In also prepared strain
Kuo
instance strap 185b. containing to
used he of units of
cytochrome alkanes the
investigate being
porphyrin-catalyzed
hydroxylation served similar
unactivated substrate, in O2 a and to and ring the and
some been in
porphyrin strapped Such displayed between bending strapped linked159,160. halves by Conden"strappedgave
transformed an
amide-linked CO
porphyrins
prepared attempt Using
methylene
strap157.
mimic and adopted of strap In is
differentiation Fe-CO Baldwin is
systems.
resonance straps) was
spectroscopy stretching et al.,
correlation Fe-C-O prepare are the is he two
(shorter strategy it the
vibrations has been observed158. different the synthetic the attached anion Acid the of porphyrins where previous ortho-positions is the ends. strap to and both opposite which the with final stretched meso-phenyl prepared step into the rings
syntheses,
initially porphyrin
porphyrin of 187 the 186.
formed
intramolecular sation ylate the to dialdehyde" unstable give he the
cyclization
position benzyl which
(Scheme gave
54).
salicylaldehyde catalyzed chain-linked This was presence was not of porphyrin
1,12-dibromododecane with after with yield.
condensation immediately 190 able in to
3,4-dimethylpyrrole-2-carboxhydrogenolysis trimethyl As of in the the orthoformate previous respective 191 was
afforded tetraacid alkyl In
bis-dipyrromethane, 23% enforce base the
189. strap the
condensed overall
"alkyl-strapped"
examples iron(II)
five-coordination six-coordinate
complex.
excess
species
formed which did not bind oxygen. Reducing the concentration of base led to an increase
172
173 of the four-coordinate was species at which -550C by underwent similar to irreversible unhindered et al.161,162), enough corners two oxidation. porphyrins, who to of were cause a of While warming attempting deformation preformed the reversible to to of room strap the were
oxygenation A a similar
observed was
temperature caused -oxo bridge formation (Scheme 55). approach with best, very in give used alkyl case, poor Wijesekera chains linking yields. porphyrin at short this very short opposite the
porphyrin. would,
Obviously
porphyrin
Instead
halves
porphyrin
assembled at each end of the strap, and only at the last step was the porphyrin 192 formed by acid-catalyzed intramolecular cyclization under high dilution conditions (Scheme 56).
Visible
and
H-NMR
spectroscopy
and
X-ray
crystallography
(Fig.
7)
all
point
to
increas-
ing distortion of the ring as the length of the strap is decreased (192, n = 11, 10, 9). A 174 chain length of nine methylene units appears to be the lower limit; attempts to prepare even more strained porphyrins with shorter straps were unsuccessful. Ligand binding to the metal complexes showed that the straps provided no steric protection.
Fig. 7. Ortep drawings of 192 (n = 9). Adapted from Ref. 162
175
6.B. Straps Containing Bulky Blocking Groups

Porphyrins oxo The bridge to logical One of strapped with In is simple alkyl chains is some the are not face bulky poor models from into for oxygen binding the increase heme heme strap, the proteins. In most cases the strap is too "floppy" and can be pushed to one side allowing \iformation. oxygen extension the addition, on to base the prevented and, group binding the strap under to to leading binding open consequently, irreversible oxidation.
incorporate of
steric encumbrance about one face. initial examples strapped porphyrin approach protein models was the cyclophane porphyrin 193 of Diekmann et al.l63). In this example steric
176
encumbrance strap, poor yield
was (5% not
provided cyclization for the used
by was as a
biphenyl delayed step heme
group until after
in the
the final
strap. step
To
ensure
tigh ly
fitting of this
porphyrin was
(Scheme an
57).
Because was
cyclization
repeated
chromatographic
purification)
porphyrin
protein
model.
Instead
anthracene
strapped
across a preformed porphyrin (194) by means of amide linkages (Scheme 58). For the
177 anthracene-heme[6,6]cyclophane ~4.5 dione of a apart. (196) second A gave axial 198 Diels-Alder the "pagoda base being 198a 195 the addition porphyrin" the two on 197 even 7,7] aromatic the possessing ring I M compound in rings an were with not I-MeIm. 198b even estimated pocket. the to to be
anthracene was
l-phenyl-triazine-2,5Binding iron(II) study
tighter
underneath and the
anthracene
observed, The were used
complexes
five-coordinate
anthracene-
heme[6,6]cyclophane
homologous[
the binding of isonitriles, CO and O2 within the pocket as models for the distal side steric effects in heme proteins164_166.
The compared effect), This but due
Fe[6,6] to flat this and to linear
cyclophane unhindered steric distal
198a
showed ( he
large
reduction cyclophane in to distal
in the
affinity ligand in
for
CO only
and a
O2 small
hemes was steric the bulky or
Fe[7,7] are face.
198b
showed the
effect side to
manifested effects heme
primarily not due While
association bound the in not and his
rate167. state, model
suggested
that limited
repulsion steric they
access bent
effects could
compounds between to postulate Baldwin benzene capped" which did not Dolphin durene did
could and that
differentiate reported his one the
isocyanide These of tilting
ligands, results CO to bound
differen iate colleagues be with the and of a "C2strap which a a may 199 to
diatomic bending strapped face absence bridge
molecules.
led in
Traylor heme a
proteins system similar in a
minor chemical significance. adapted above 160, u-oxo his prevent porphyrin (Scheme of the by synthesis 59)160. two ligands An extra such even a prepare ring not Although as more series structurally resulted or bulky of I-MeIm
porphyrin prevent and
linkages
"floppy"
six-coordination
pyridine
formation. have (201)
strap,
incorporating with
naphthalene ring as in 200, was no more successful. colleagues161,162) one face prepared (Scheme strapped of porphyrins iron using group protecting 60). Incorporation stan-
dard methods168 gave the corresponding heme complexes 202a-c. The crystal structure
of that
the
hemin from 201c 201c 201b
chloride
derived The
from
202a also in
(Fig. spectra the data plane of
8) for
showed the
considerable free base base the tighter CO, are
distortion porphyrins while moiety 5/5 been
of the in and
the
7/7-
porphyrin some derivative

7/7-base
planarity169. distortion essentially closer 201a. their of to is is and to
optical
1
indicate the
-4/4
porphyrin
exists flat. he heme
durene-5/5 suggest than the in
free that the
201b, durene capped have and
H-NMR
porphyrin with of in the the
analogs with binding Me2Im) durene
The
derivatives
durene and
porphyrins
studied The (1,2the reasons,
respect to
interaction side
imidazoles,
isocyanides, hemes
O2114170. within
constants the series
1,5-dicyclohexylimidazole differences
(DcIm) plane
1,2-dimethylimidazole similar for steric
unhindered despite
four-coordinate porphyrin
distortion;
these imidazoles do not coordinate on the capped (or distal) side of the heme. The size of
179
180
Fig. 8. A SNOOPI diagram (E. K. Davies, plotting rou ine, 1984, Chemical Crystallography Laboratory, 9 Parks Road. Oxford. England) of the hemin chloride of 202a (50% probability contours for all atoms; hydrogen atoms have been omitted for clarity; the dashed bonds are used to distinguish between the "strap" and the porphyrin skeleton)
202
the (TMIC)
distal and
cavity restrictive of
was distal
examined (t-BuNC), environment isocyanide.
using which of The
the the
bulky in durene-4/4
isocyanides, their spatial system,
tosylmethylisocyanide requirements. inhibited obtained The the from
t-butylisocyanide either
differ
extremely coordination
however, complex
Fe"(durene-7/7)(DcIm)
202c exhibits a reduced overall affinity for CO relative to simple flat, open hemes; this is
181 manifested steric effect in as a a from depressed result of association the rate for The CO, and was and CO strain a interpreted170
-4/4
as
distal from
durene-cap. dissociation of the
durene-5/5 for steric
systems the by
derived
202a and 202b also show reduced CO affinities compared to open hemes, but this results predominantly Fe(P)(DcIm)CO Me2Im) skeletal 202b relative heme values) distal within bind B to (or O2 increased because to rates proximal from induced six-coordinate the of porphyporphyrin relative of to CO (M their of complexes O2
rin plane distortion. The five-coordinate hemes 202a B - 202c B (B = DcIm or 1,2reversibly A less similar extents, arises all implying from negligible 202a steric effect distortion. 10-fold reduced distorted his B is affinity for CO hemes) B that the in a base distorted by the system. show with Fe-O2 B complex the
other 202a to
proximal
discrimination kco/k2 functions electronic the strap cavity significant was and
within
severely 202c hemes stabilizing (as face of CO, O2 the O2 the
Significantly, higher amide of polar concept and was give showed to the displayed binding straps heme
five-coordinate ratios in
complexes relative the distal
considerably the
encumbered This pocket strategy one
incorporate
environments.
entirely
consistent
interactions affinity a
binding
moiety 58) to 9) bind the
increasing used no Fe" no constant of 204 257 to free
the heme toward O2, relative to CO114'170. The phane. the greatly same The synthetic shown of free and Scheme porphyrin (Fig. bulky cyclobetween 203 with steric adamantane strap group crystal the and across l,3-adamantane[6,6] complex
structure171 porphyrin; CO the no
isocyanides For the CO
reduced
rates.
However and
adamantane
strap
differentiation In Chap. et the strap
between to a
binding. of
controlled 259 by (see Traylor formashorter 204
by the association rate, dissociation not being increased by the steric effects of the strap. contrast 6.C.), ligand strapped evidence and bases behaviour of to either iron(II) strain pyridine or singly pyridine-[5,5] cyclophane prepared
al.172,
showed of
internal
external is
iron-pyridine
complex the
tion. Indeed even the binding of CO to 204 failed to induce pyridine ligation even though binding in this CO case porphyrins to prevent synergistic. binding Obviously and induces sufficient internal compound
behaves more like the anthracene and adamantane cyclophanes 198 and 203. The
Fig. 9. Perspective view of a l,3-adamantane[6,6] cyclophane porphyrin. Adapted from Ref. 171
182
pyridine between
heme in CO
204 and
displays O2
severe than
steric rates. other
hindrance Furthermore models, the
to the
both 204
O2
and a binding
CO
binding, being
which
is
manifested
lower
association binding have
shows
greater ratio
differentiation possibly in
lower of
due to enhanced binding of O2 in the tight polar pocket114. Dolphin and Morgan173 prepared series strapped porphyrins illustrated Fig. 10 and Scheme 61. As a consequence of postponing porphyrin ring formation (a
183
Fig. 10. Ortep drawings of a strapped porphyrin containing a thioether linkage. Morgan, B., Dolphin, D., Einstein, F. W. B., Jones, T., manuscript in preparation specific example is given in Scheme 61) till the later stages on the synthesis, (i) a range of strap (ii) ester strap lengths linkages have are available, may (iii) some be of which stability 10), 61) as may is lead obtained 205 and potential to any distortion polar due to for of the 206 the due porphyrin, to amide in and or the strap. catalase hydrocarbon straps and employed, (Fig. precluding phenol effects
increased (Scheme
hydrocarbon groups174 c,
Compounds
including been
thioethers
quinone
prepared
models
cytochrome
and photosynthetic charge separation, respectively.
184
6. C Straps Containing Interactive Groups

The incorporation of potential ligands into the porphyrin strap has three advantages, (i) A stoichiometric amount of ligand is built into the system, ensuring five-coordination without the addition of external ligand. In the case of nitrogen bases, mixtures of six- and four-coordinate complexes are avoided. (H) For ligands which bind poorly to iron(II) (e.g. thiolate), coordination would be favoured by constraining the ligand into a position suitable for binding to the metal, (iii) Because the strap is fixed to the porphyrin and the ligand in two positions, complications due to ligand replacement or dissociation will be minimized. The strapped-porphyrin approach is also useful for orientating other interactive groups (e.g., metal binding sites, electron donor/acceptor groups) into specific geometries with respect to the porphyrin.
185
Battersby substituted 38% yield is corresponding syntheses (Scheme
et pyridine
al.
have ligands175. diol 62). in suitably
prepared Reac ion gave 11176). 207 The
a of the A
series the
of
strapped pyridine a P450 was
porphyrins chloride straps was under
bearing 180 in 208a-c
variously with up of the to these similarly with
porphyrin of
bis-acid crystalline model reacted
pyridine (Scheme shown A
ester-linked structure cytochrome
molecular
side-product prepared high
Fig.
63)177.
functionalized
diol
211
dilution
the bis-acid chloride of mesoporphyrin II (180) to give the strapped porphyrin 212 in 25%
186 yield. group the iron(II) whose monoxy 450 nm. Several binding formed bind ether face a two The with S-acetyl species. visible The protected-sulfur potassium group On was derivative cleaved to spectrum spectrum spectrum strapped in a ion of 213 with CO a a was iron dimsyl obtained sodium the hyper CO major Soret by to iron(II) band also displacement reduction to produce species with an of the the 214 of the are 217 IIA the iron(II) was the tosyloxy state, formed carbonband at
thioacetate. exposure
After
insertion
and
five-coordinate
six-coordinate
absorption P450
13
reproduced split the

13
characteristics supported which
cytochrome
intense
C-NMR
complex been
RSFeII-CO capable of of
formulation. binucleating metal ions porphyrins proximity. porphyrin Apart over have The e her ring) from one prepared, the group the bind Oxygen close (in the 64). control a "crowned" 216 to and its face a of metal porphyrin IA or Chang178, 215, may (in the the the crown iron(II) the
by the addition of transition also exerts bulky metal ring) some Iigands to
bis-amino crown
bis-acid chloride capability For the bind on then
cation
diaza-18-crown-6 complexes, of the
(Scheme steric (e.g., give
binding only may
porphyrin.
1-triphenylmethylimidazole) five-coordinate species.
unhindered under
porphyrin
crown to give a reasonably stable oxygen species (t1/2 > 1 hr at 250C in DMA).
Recently, he and rate (Scheme cations
another of The
crown-strapped 225b (see corresponding Bimetallic indicated crown fluorescence
porphyrin Scheme
219 67) were
similar with is a
to the
217
has host for at
been crown for with the
prepared ether both the
by 218
condensation 65)179. e.g. of Cu", cationic salts The
bis-amino and, salt
metalloporphyrin quenching of was the
potential
anionic guest perchlometal
species. FeIII, diamines of have 66). acid provided compound
complexes attachment and the of of to
prepared perchlorate has also
paramagnetic porphyrin out wi h (221) 10% and by
observed.
Studies
site and complexation of the ammonium species at the crown ether. combination who acetic 222 This (Scheme e her porphyrin been carried 220 and Bogatskii by pyrrole with group I, yield two in the II et al.180, prepared Condensation or the is reac ion tetra-crown reported wo-tetra(benzo-18-crown-6)porphyrin 4'-formylbenzo-18-crown-6 porphyrin 223 in 4% tetra(3,4-dihydroxyphenyl)porphyrin form complexes with transition 223
routes refluxing dichloride tively. metals.
ether
respec-
The ton et
combination al.1B1 at 55 The

0
of
crown ether
ether 224
and with
porphyrin 226 the
has was
recently prepared
been by
extended
by
Hamilof b the in
macrotetracyclic under high
cryptand dilution
condensa ion porphyrin 225a,
biphenyl-linked pyridine
bis-crown C
di-p-nitrophenyl (45-54%
ester after
conditions
chromatography).
Reduc-
tion to the tetra-amine 227 was effected by treating the zinc complex with diborane
188
followed selective within
by
demetallation binding:
+
(Scheme transition
67). metal (n =
This
multisite are within
complexing bound the the by by
species the cavity. upfield
is
capable and of That
of alkyl the
substrate salts, cavity
cations 8-10),
porphyrin
diammonium the
H3N(CH2)nNH3+ indeed
central large
binding
does
occur
was
evidenced
shifts
methylene protons due to the shielding effects of the porphyrin and biphenyl rings.
189
A mimic The cine the
copper the 228 in
binding
site
has was
been a of
covalently of the
attached derivative for a
to
porphyrin of obtainable than to 231 in
in
an from
attempt
to
EPR high of
spectral strap yield. the to
characteristics Because the of
iron-copper
site
cytochrome copper
oxidaseI82 phthalylglysite,
copper-binding strap was (230) and and a by
bis-thiazole need the the a sulfide ions of
229,
non-square-planar ring rather with
binding XII
attached under into
one side dilution 68). to The et
porphyrin 229 strapped could coupling a
opposite 72% a to
corners. bis-acid after the spin was a
Condensation chloride porphyrin iron(III) chromatography
diaminothiazole gave give al.183, Metal
mesoporphyrin
high the
porphyrin complex
yield into high centers
(Scheme copper(II) EPR.
be metal
differentially the
introduced containing two metal approach
strap ion.
dinuclear
extent
between
investigated
Gunter
used
somewhat
different
prepare
similar Fe/Cu strapped porphyrin (Scheme 69). Condensation of the tetramethyldipyr-
190
romethane ers 235. were
232
wi h
o-nitrobenzaldehyde After by reduction
(53), to
followed the
by
oxidation 233
afforded was the
the the
5,15-meso(orthoatropisomers condensed gave species and of yield dioxide. the with of porphyrin
nitrophenylporphyrin. separated of model iron
amino and yielded of
derivative
chromatography. chloride) copper and
The (234), the and
cc,a-isomer introduction
finally ligands
2.6-pyridylbis(4'thia-5'-pentanoyl Insertion As esh185,186 tersby bis-acid on a and
strapped
bridging
the type 236, whose magne ic properties were investigated184. for photosynthetic a give electron-transfer porphyrin. 237 porphyrins quinones d and Using 238 239a, that in b the were with systems, the 7 reacted boron Sanders wi h and with 15% lead trichloride quinone GanBatII the to have group, chloride strap on prepared (180) to were that quinone-capped deriva ives strapped to the the c, the 70). approach
1.4-dialkoxybenzene length which (Scheme
mesoporphyrin afforded binds
depending 'H-NMR perpen-
Deprotection 239
hydroquinones studies the the metal
oxidized complexes theretore
magnesium and
suggest
carbonyl are
ion
quinone
porphyrin
chromophores
dicular187.
Since oxygen sponding auenchine parallel nesium
zinc ligands, zinc is approach
is
exclusively
five-coordinate binding free of especially base is the
in the
porphyrins chromophores with and added zinc is are the with but
and is 239e,f much
has
low in
affinity the where
for correclose, mag-
intramolecular complexes in the 239c.d of the of the
lessened
239e,f
ligands
present. complexes reduced for The
Fluorescence the
observed of
239a,b
chromophores where
possible,
complexes binding
chromophores in diols 239c,d 240
perpendicular"*'. quenching 180 gave
quenching is similar strapped
is more efficient for the longer chain 239b. f than for the shorter chain 239a. e; because of intramolecular High chromophores the bipyridyl efficiency the bipyridyl for both chain lengths. dilution coupling porphyrins 241 (Scheme 71) in 40-50% yield189 191 Treatment with iodomethane fur-
191
192
nished donor potential reduced was
the
methylviologen and
strapped an
porphyrins acceptor of
242.
The
close
proximity dication) of 241 to by 243. give the into
of and the
an 242 two
electron this a were It radical of the at
(porphyrin) ~200 fold that et II
electron Indeed to
(methylviologen emissions methylviologen electron and
makes
photosyn hetic
model.
fluorescence an excited a
relative efficient have with 72).
mixtures of
unstrapped
porphyrin.
assumed Hamilton
trapping also
occurred complex diol two
cations of the connected chromophores. al.192, diacid 244 (Scheme prepared 180 close with binuclear the by of condensation Reaction the of mesoporphyrin strapped resulted in chloride The bipyridyl metal the
porphyrin 245
Ru(byp)2Cl2
followed proximity
insertion metal
porphyrin
4 is reflected in both the luminescence and electrochemical properties of the complex.
centers,
estimated
6.D. Doubly-Strapped Porphyrins

We have oxo face. bridge Steric of already seen formation Amundsen and his and to if encumbrance that sterically encumbered porphyrins any on and four-coordinate both faces of Vaska148 and have on species the in porphyrin, may may still binds in the as be susceptible to on he "bis-pocket" a solution oxygen this open oxidaprepare of salicylformed
porphyrin
systems
Suslick149, used a
prevent of In the TPP a and
bimolecular to of then
tion pathway. Momenteau TPP derivatives was 246a-e Baldwin's aldehyde derivatives colleagues two straps with a "strapped" combination ring193. approaches strategy sodium ring salt was having reacted give each porphyrin of reminiscent
"capped"
porphyrin variety
syntheses159-160), dibromoalkyl 247. The
p-(dibromoalkyl)benzene
chain-linked
dialdehydes
by condensing the dialdehydes with pyrrole in refluxing propionic acid (Scheme 73).
193 After in low minant formation (Scheme removal overall isomer. of 74). of yield. To the polymeric The bridges (10% Alkyla ion by followed increase materials, the was yield three of the until isomers cis-linked more after (249) dibromo led to were product interesting the was obtained 248c was cross by chromatography the predoisomers, and dilution porphyrin
unwanted
adjacent delayed and the
often
trans-linked from under
porphyrin-forming obtained to isolation 246 of provide the
condensation pyrrole high hree tetra(o-hydroxy-
Tetra(o-methoxyphenyl)porphyrin yield) with (250).
o-methoxybenzaldehyde phenyl)porphyrin in DMF at 100C,
demethylated the
derivatives
chromatography
isomers 248. In this case the major product of each reaction was atropisomers since the conditions of the condensation would lead to equilibra ion.
he desired cross trans-
linked isomer 248a. The starting porphyrin 250 was used as a mixture of the four possible
The tion and of is
degree the iron easily
of
steric
encumbrance The In contrast do
is the
illustrated cis-linked other not
by
the
rates 248c where
of has both of at t 7-54
metallation one faces face
and
oxida-
various
isomers.
adjacent While inhibit
isomer
unhindered hindered, bases to 25 or For the oxida0
metallated. insertion the
isomers,
are
undergo diatomic the tion under The metallation try. paralleling A hematin of O2
reluctantly. chains cross is isomers
preventing isomer
ligation he to
nitrogenous room for in oxidation seconds toluene is
molecules, derivative the (1 less atm),
irreversible minutes u-oxo the
oxidation 248a
temperature. for at 11-25 only
four-coordinate
iron(II) FeIII(P)OH hindered t1/2
trans-linked 1.5-10.5 to the of
compared complex.
Similarly, iron(II)
for
oxidation picket-fence small
six-coordinate show in the the their iron free
complex effects and have
min
for the cross trans-linked isomer compared to 1.5-12 min for the other two isomers194. basket-handle and the binding on earlier studies and of porphyrins but of on been the dramatic redox not during chemismade195' and al. . hat zinc The with do molecules studies has in the coordination been magnesium Zhilina was et
Detailed
the
electrochemistry
complex base, by (142) of The
electrochemical porphyrin
complexes of 192 and 201196. similar doubly-strapped of room at reported a,b,a,b triglycolic not cause atropisomer dichloride significant meso-tetra(o-aminophenyl)porphyrin temperature of presence atropisomer. acylated
pyridine,
conditions
isomerization
doubly-strapped
porphyrin
251 was obtained in 32% yield after chromatography (Scheme 75).
In a units. yielded desired
contrast Thus, a cross
to
the
sequential to prepare of the
introduction a and bis-aldehyde
of
bridging with
straps, pyrrole was and
Weiser in
and
Staabl98 propionic
used acid The its
one-step
synthesis mixture of
porphyrin polymers, obtained
sandwiched 252 in and three ~0.1%,
between
two refluxing
parallel
quinone
condensation trans-linked symmetric

1
oligomers H-NMR
doubly-strapped easily oxidation
porphyrins. identified then by
porphyrin,
characteristic
spectrum.
Deme hylation
yielded
the desired bis-quinone porphyrin 253 (Scheme 76).
A globin, of the
further
refinement models of system a
to
he
production different base steric
of
heme one
protein As
models for by
was
the the
synthesis or proximal strap
of face
doubly-strapped natural
containing nitrogen the while
straps.
models would
hemoglobin second
myowould
incorporation
into
strap
simulate the
encumbrance
provided
mimic the distal, oxygen-binding face.
Momenteau's compounds tion lent on of of in
route which an
to
doubly-strapped base gave or by to was (250) a
porphyrins incorporated (mixture of (254) tic (5% of two
was into one four
easily of
adapted the wi h were desired
to one
produce Condensaequivadepending This transsimilar in of this 78). both
axial
straps199' porphyrins,
tetra(o-hydroxyphenyl)porphyrin 1.12-dibromododecane adjacent reacted 257 was were insertion (255), with was
isomers) groups the
mixture
singly-linked and yield) amide and

1
whether isomer 259 the
opposite preparative from the
meso-phenyl 256 overall by
linked. cross A
mixture linked case porphyrin Following
3,5-bis(3-bromopropyl)pyridine
isolated tied and
(Scheme linkages
77). (142); spectra
prepared
a,b.a,(3-tetra(o-aminophenyl)porphyrin porphyrin visible skeleton absorption H-NMR
straps iron
(Scheme
reduction,
compounds were consistent with a five-coordinate high spin (S = 2) iron(II) complex.
The by laser of
rate constants for the flash ca. of photolysis. 10 in he The O2
association O2 affinity
and of
dissociation of O2 and CO were determined the "amide" koffO2 linked 4 vs to system 0.5 the s_l). was This higher than in N-H
that of the "ether" linked compound p 18.6 vs 2 torr) as a result of a difference of a factor stability dissociation rates (10~4 was increase of the the "amide" oxygenated species attributed presence
group and the possibility of hydrogen-bonding with the terminal oxygen atom. The low
temperature quivalence of
(-27C)
H-NMR
spectrum
supported
this
hypothesis,
the
observed
ine-
he pyrrole protons as well as
he shifts of the amide protons suggesting a
preferred orientation of the oxygen molecule towards the amide N-H groups200. To better model the hemoglobin and myoglobin active sites a doubly strapped heme 260 was prepared incorporating a pendant imidazole (Scheme 79)201. 260 was capable of binding oxygen to give a rela ively stable oxygenated species (lifetime was about one day in dry toluene under 1 atm O2). The kinetics of O2 and CO binding have been determined and initial comparisons with the comparable "pendant pyridine" porphyrins show: (i) (ii) O2 and CO combina ion rates are practically constant in the three pendant base porphyrins, and a reduction in konO2 in the imidazole porphyrin due to a combination of hydrogen bonding with the amide N-H and the greater basicity of imidazole over pyridine. Comparison of the pendant imidazole model with myoglobin or isolated hemoglobin chains shows that the model reacts 10 times faster with O2 and that the dissociation rate is approximately 100 times faster than in the natural systems. With the availability of the differentially protected coproporphyrin I 261, Battersby and Hamilton adapted heir syntheses to the production of doubly-strapped porphyrins
(Scheme ridine esters 263 with to difficult and so
80)202. the the acid the
Reaction chloride metal
of
the
bis-acid porphyrin was after be a
chloride 262 by
261
with
3,5-bis(3-hydroxypropyl)pyof the found strap. of min the of to the at benzyl diol be to with the was basis 15 was into anthracene
yielded give
pyridine-strapped formation inserted the to doubly-bridged was furnished judged In DMF
(33%). Iron of = of
Hydrogenolysis insertion the on 2) the
followed 264 the high with
condensation
porphyrin iron(II)
(27%).
introduc ion species spin a t1/2 stable was (S
pyridine
Reduction visible to (t1/2 Such This room
aqueous gave in
dithionite was an
which
absorption oxygen temperature and was
spectrum
five-coordinate. species CO by
Exposure formed O2.
oxygenated
compound O2 six of
approximately by passing
CH2Cl2of to the be the
more species times
oxygenated accomplished significant CO-porphyrin imidazole (57%).
approximately 2 regeneration cycles in The reported203'. the esters yield cycles and contrast further As O2-CO
h at 20C). The could repeated
could be
displaced without
solution,
oxygenated resistance of give
passage
irreversible complexes ligand 261 was has was removal reacted oxygen being was
oxidation.
unhindered an
displacement recently with benzyl the in N22% four before ca. rigid before gave he
of CO by O2. refinement before, diol 263 with diol The the to incorporating the porphyrin the was The been of the with differen ially chloride, The complex (by occurred. protected coproporphyrin After 267 chloride of the still 268 268a reacted
anthracene
265 bis-acid capable
treatment imidazole 81).
oxalyl 266. iron(II)
substituted of
doubly-bridged reducing t1/2
porphyrin the for was
obtained possible species floppy,
(Scheme
reversible
binding, was more as
oxygenation-deoxygenation irreversible that oxidation the a he
pressure)
significant
oxygenated somewhat were or
24 h at room temperature in DMF solution. Recognizing straps (Scheme imidazole pendant-imidazole 1,5-disubstituted bis-acid chloride strap imidazole of the containing 81)203). 268b with prepared porphyrin
Coupling
1,5-bis(4-hydroxybutyl)
l,5-bis(3-hydroxypropyl)-
anthracene-strapped
doubly-bridged systems 269a, b in 23% and 6% yield. Distortion of the porphyrin ring
198
from the ture. dation
planarity iron(II) Ten was
to
accommodate could and
the
shorter bind cycles 20%
strap oxygen could
was in be
believed DMF
responsible at
for
the
low
yield of 269b and also for the lesser stability of the oxygenated iron(II) species. For 269a, complex reversibly only solution occurred ambient after 2 temperaoxiin days oxygenation-deoxygenation significant, performed before irreversible
irreversible
oxida ion
solution. Acknowledgements. This work was supported by the United States National Institute of Health (AM 17989) and the Canadian Natural Sciences and Engineering Research Council.
7. List of Abbreviations
acac AQ bipy 1-n-Bulm 4-t-BuIm t-BuNC BO CO Cys cyt DCIM DDO DMA acetylacetonate Anthraquinone bipyridyl 1-n-Butylimidazole 4-t-Butylimidazole t-Butvlisocyanide Benzoquinone Carbon monoxide Cysteine cytochrome 1,5-Dicyclohexylimidazolc 2,3-Dichloro-5,6-dicyano-l,4benzoquinone N1N-DimethyIacetamide DMF DMSO DNA ee Et3N EXAFS N1N-DimethyIformamide Dimethylsulfoxide Deoxyribonucleic acid enantiomeric excess Triethylamine Extended X-Ray Absorption Fine Structure H2(OEP) Octaethylporphyrin general porphyrin H2(P) H2(TAP) Tetra(p-methoxyphenyl)porphyrin H2(T(OH)PP) Tetra(o-hydroxyphcnyl)porphyrin H2(TPP) Tetraphenylporphyrin
H2(TTP) His Hm Im MCD I-MeIm l,2-Me2Im MeOH Met NQ
Tetra(p-tolyl)porphyrin Histidine Heme Imidazole Magnetic Circular Dichroism I-Methylimidazole 1,2-Dimethylimidazole Methanol Methionine Naphthoquinone
phth piv THF THT TMIC Tos Tr l-trityllm Tyr
phthaloyl pivalamido Tetrahydrofuran Tetrahydrothiophene Tosylmethylisocyanide Tosylate Trityl I-Tritylimidazole Tyrosine
8. References
Hemoglobin and Oxygen Binding (Ho, C, Ed.), Elsevier Biomedical, New York 1982 Mathews, F. S.: Prog. Biophys. Mol. Biol. 45, 1 (1985) Hatefi, Y.: Ann. Rev. Biochem. 54, 1015 (1985) Frew, J. E., Jones, P.: Adv. Inorg. Bioinorg. Mech. 3, 175 (1984) Murray, R. T.. Fisher. M. T., Debrunner, P. G., Sligar. S. G.: Top. Mol. Struct. Biol. 6 (Metalloproteins, Pt. 1). 157 (1985) 6. The Porphyrins (Dolphin, D., Ed.), Academic Press, New York, Vol. VII, Part B, 1978 8. NATO Adv. Study Inst. Ser., Ser. C, 89 (The Biological Chemistry of Iron) (1981) 8. Kao, O. H. W., Wang, J. H.: Biochemistry 4, 342 (1965) 9. Hammond, G. S., Wu, C H. S.: Adv. Chem. Ser. 77, 186 (1968) 10. Cohen, I. A., Caughey, W. S.: Biochemistry 7, 636 (1968) 11. Latos-Grazynski. L., Cheng, R.-J., La Mar, G. N., Balch, A. L.: J. Am. Chem. Soc 104, 5992 (1982) 12. Holquist. D. E., Saunes, L. J., Juckett, D. A.: Curr. Top. Cell. Regul. 24, 287 (1984) 13. Brunori. M., Falcioni, G., Fioretti, E., Giardina, B., Rotilio, G.: Eur. J. Biochem. 53, 99 (1975) 14. Fee, J. A.: Metal Ion Activation of Dioxygen (Ed. Spiro, T. G.), Wiley Interscience. 209-237 (1980) 15. Phillips, S. E. V., Schoenborn, B. P.: Nature (London) 292, 81 (1981) 16. Shaanan, B.: Nature (London) 296, 683 (1982) 17. Perutz, M. F.: Scientific American 239{6), 68 (1978) 18. Brault, D., Rougee, M.: Biochemistry 13, 4591 (1974) 19. Brault, D., Rougee, M.: ibid. 13, 4598 (1974) 20. Scheidt, W. R., Reed, C A.: Chem. Rev. 81, 543 (1981) 21. Stynes, D. V., Stynes, H. C, James, B. R., Ibers, J. A.: J. Am. Chem. Soc 95, 1796 (1973) 22. Anderson, D. L., Weschler, C J., Basolo, F.: ibid. 96, 5599 (1974) 23. Almog, J., Baldwin, J. E., Dyer, R. L., Huff, J.. Wilkerson, C J.: ibid. 96, 5600 (1974) 24. Brinigar, W. S., Chang, C K.: ibid. 96, 5595 (1974) 25. Wagner, G. C, Kassner, R. J.: ibid. 96, 5593 (1974) 26. Traylor, T. G., Chang, C. K., Geibel, J., Berzinis, A.. Mincey, T., Cannon, G.: ibid. 101, 6716 (1979) 27. Gibson, Q. H.: Prog. Biophys., Biophys. Chem. 9, 1 (1959) 28. Basolo, F., Hoffman, B. M., Ibers, J. A.: Acc Chem. Res. 8, 384 (1975) 29. James, B. R.. Addison, A. W., Cairns, M.. Dolphin. D., Farreli, N. P.. Paulson, D. R., Walker, S.: Fundamental Research in Homogeneous Catalysis (Tsutsui, M.. Ed.), Plenum Press: New York, Vol. 3, p. 751 (1979) 30. Wang, J. H.: Ace Chem. Res. 3, 90 (1970) 31. Leal, O., Anderson, D. L., Bowman, R. G., Basolo, F., Burwell, R. L.: J. Am. Chem. Soe 97, 5125 (1975) 32. Collman, J. P.: Ace Chem. Res. 10, 265 (1977) 33. Jones, R. D., Summerville, D. A., Basolo, F.: Chem. Rev. 79, 139 (1979) 34. Smith, P. D., James, B. R., Dolphin, D. H.: Coord. Chem. Rev. 39, 31 (1981) 1. 2. 3. 4. 5.
200 36. Traylor, T. G.: Acc Chem. Res. 14, 102 (1981) 37. Bogatskii, A. V., Zhilina, Z. I.: Russ. Chem. Rev. 57, 592 (1982) 38. Collman, J. P., Halpert, T. R., Suslick, K. S.: Metal Ion Activation of Dioxygen (Spiro, T. G., Ed.), Wiley: New York, p. 1 (1980) 39. Lautsch, V. W., Wiemer, B., Zschenderlein, P., Kraege, H. J.. Bandel, W., Gunther, D., Schulz, G., Gnichtel, H.: Kolloid. Z. 161, 36 (1958) 40. Losse, G., Muller1 G.: Hoppe-Scyler's Z. Physiol. Chem. 327, 205 (1962) 41. Van der Heijden, A., Peer, H. G., Van den Oord, A. H. A.: J. Chem. Soc., Chem. Commun., 369 (1971) 42. Warme, P. K., Hager, L. P.: Biochemistry 9, 1599 (1970) 43. Momenteau, M., Rougee, M., Loock, B.: Eur. J. Biochem. 71, 63 (1976) 44. Castro, C E.: Bioinorg. Chem. 4, 45 (1974) 45. Molokoedov, A. S., Fillippovich, E. I., Mazakova, N. A., Evstigneeva, R. P.: Zhur. Obshch. Khim. Ed. Engl. 47, 1070 (1977) 46. Kazakova, N. A., Radyukhin, V. A., Luzgiva, V. N., Filippovich, E. I., Kamyshan, N. V., Kudryavtseva, E. V., Evstigneeva, R. P.: ibid. 52, 1896 (1982) 47. Momenteau, M.. Loock, B.: Biochim. Biophys. Acta 343, 535 (1974) 48. Selve, C, Niedercorn, F.. Nacro, M., Castro, B., Gabriel, M.: Tetrahedron 37, 1893 (1981) 49. Selve, C, Niedercorn, F., Nacro, M., Castro, B., Gabriel, M.: ibid. 37, 1903 (1981) 50. Gabriel, M., Grange, J., Niedercorn. F., Selve, C, Castro, B.: ibid. 37, 1913 (1981) 51. Goulon, J., Goulon, C, Niedercorn. F.. Selve, C, Castro, B.: ibid. 37, 2707 (1981) 52. Chang. C K., Traylor, T. G.: Proc Natl. Acad. Sci. U.S.A. 70, 2647 (1973) 53. Chang, C K., Traylor, T. G.: J. Am. Chem. Soc 95, 5810 (1973) 54. Chang, C K., Traylor, T. G.: ibid. 95, 8475 (1973) 55. Brinigar, W. S., Chang, C K., Geibel, J., Traylor, T. G.: ibid. 96, 5597 (1974) 56. Geibel, J., Chang, C K., Traylor, T. G.: ibid. 97, 5924 (1975) 57. Dolphin, D., Hiom, J., Paine III, J. B.: Heterocycles 16, 417 (1981) 58. Traylor, T. G., Campbell, D., Sharma, V., Geibel, J.: J. Am. Chem. Soc 101, 5376 (1979) 59. Traylor, T. G., White, D. K., Campbell. D. H., Berzinis, A. P.: ibid. 103, 4932 (1981) 60. Traylor, T. G., Mitchell, M. J., Cicone, G. P., Nelson, S.: ibid. 104, 4986 (1982) 61. Traylor, T. G., Tatsuno, T., Powell, D. W., Cannon, J. B.: J. Chem. Soe Chem. Commun., 732 (1977) 62. Traylor. T. G., Berzinis, A. P.: J. Am. Chem. Soe 102, 2844 (1980) 63. Tabushi, I., Sasaki, T.: Tetrahedron Lett. 23, 1913 (1982) 64. Tabushi, I., Kugimiyua, S., Kinnaird, M. G., Sasaki, T.: J. Am. Chem. Soe 107, 4192 (1985) 65. Tabushi, I., Kugimiya, S., Sasaki, T.: ibid. 107, 5159 (1985) 66. Denniss, J. S., Sanders, J. K. M.: Tetrahedron Lett., 295 (1978) 67. Boxer, S. G., Wright, K. A.: J. Am. Chem. Soe 101, 6791 (1979) 68. Momenteau, M., Loock, B., Bisagni, E.. Rougee, M.: Can. J. Chem. 57, 1804 (1979) 69. Callot, H. J.: Tetrahedron, 899 (1973) 70. Lavalette, D., Tetreau, C, Momenteau, M.: J. Am. Chem. Soe 101, 5395 (1979) 71. Lavalette, D., Momenteau, M.: J. Chem. Soe, Perkin Trans. 2, 385 (1982) 72. More, K. M., Eaton, S. S., Eaton, G. R.: Inorg. Chem. 20, 2641 (1981) 73. Damoder, R., More, K. M., Eaton, G. R., Eaton, S. S.: J. Am. Chem. Soe 105, 2147 (1983) 74. Damoder, R., More, K. M., Eaton, G. R., Eaton, S. S.: Inorg. Chem. 22, 2836 (1983) 75. Collman, J. P., Brauman, J. I., Doxsee, K. M., Halbert, T. R., Bunnenberg, E., Linder. R. E., LaMar, G. N.. Del Gaudio, J., Lang, G., Spartalian, K.: J. Am. Chem. Soe 102, 4182 (1980) 76. Mashiko, T., Reed, C A., Haller, K. J., Kastner, M. E., Scheidt, W. R.: ibid. 103, 5758 (1981) 77. Walker, F. A.: ibid. 102, 3254 (1980) 78. Walker, F. A., Benson, M.: ibid. 102, 5530 (1980) 79. Santon, R. J., Wilson, L. J.: J. Chem. Soe, Chem. Commun., 359 (1984) 80. Molinaro, F. S., Little, R. G., bers, J. A.: J. Am. Chem. Soe 99, 5628 (1977) 81. Goff, H.: ibid. 102, 3252 (1980) 82. Traylor, T. G., Mincey, T. C Berzinis, A. P.: ibid. 103, 7084 (1981) 83. Collman, J. P., Groh, S. E.: ibid. 104, 1391 (1982) 84. Buckingham, D. A., Rauchfuss, T. B.: J. Chem. Soe, Chem. Commun., 705 (1978)
201 86. Smith K. M., Bisset, G. M. F.: J. Chem. Soc., Perkin Trans. 1, 2625 (1981) 87. Kong, J. L. Y., Loach, P. A.: J. Heterocycl. Chem. 17, 737 (1980) 88. Mcintosh, A. R., Siemiarczuk, A., Bolton, J. R., Stillman. M. J., Ho, T.-F., Weedon, A. C: J. Am. Chem. Soc 105, 7215 (1983) 89. Mcintosh, A. R., Siemiarczuk, A., Bolton, J. R., Stillman, M. J., Ho, T.-F.. Weedon, A. C: ibid. 105, 7224 (1983) 90. Wang, C-B., Tien, J. T., Lopez, J. R., Lui, Q.-Y., Joshi, N. B., Hu, Q.-Y.: Photobiochem. Photobiophys. 4, 177 (1982) 91. Joshi, N. B., Lopez, J. R., Tien, H. T., Wang. C-B., Lui, Q.-Y.: J. Photochem. 20, 139 (1982) 92. Tabushi. I., Koga, N.. Yanagita, M.: Tetrahedron Lett., 257 (1979) 93. Wasielewski, M. R., Niemczyk, M. P.: J. Am. Chem. Soc 106, 5043 (1984) 94. Wasielewski, M. R., Niemczyk, M. P., Svec, W. A., Pewitt, E. B.: ibid. 107, 1080 (1985) 95. Joran, A. D., Leland, B. A.. Geller, G. G., Hopfield, J. J., Dervan, P. B.: ibid. 106, 6090 (1984) 96. Nishitani, S., Kurata, N., Sakata, Y.. Misumi, S., Migita, M., Mataga, N.: Tetrahedron Lett. 22,2099 (1981) 97. Mataga, N., Karen, A., Okada, T., Nishitani, S., Kurata, N., Sakata, Y., Misumi, S.: J. Phys. Chem. 22, 5138 (1984) 98. Nishitani, S., Kurata, N., Sakata, Y., Misumi, S., Karen. A., Okada, T., Mataga, N.: J. Am. Chem. Soc 105, (1983) 99. Moore, T. A., Gust, D., Mathis, P., Mialocq, J.-C, Chachaty, C, Bensasson. R. V., Land, E. J., Doizi, D., Liddel, P. A., Lehman, W. R., Neme h, G. A., Moore, A. L.: Nature (London) 307, 630 (1984) 100. Maiya, G. B.. Krishnan, V.: Inorg. Chim. Acta 77, L13 (1983) 101. Kobayashi, N., Akiba, V.. Takatori, K., Veno, A., Osa, T.: Heterocycles 19, 2011 (1982) 100. Eshima, K., Matsushita, Y., Sekine. M., Nishide, H., Tsuchida, E.: Nippon Kayaku Kaishi. 214 (1983) 101. Lown, J. W., Joshua, A. V.: J. Chem. Soc., Chem. Commun., 1298 (1983) 102. Hashimoto, Y., Lee, C-S., Shudo, K., Okamoto, T.: Tetrahedron Lett. 24, 1523 (1983) 103. Collman, J. P., Gagne, R. R., Halbert, T. R., Marchon, J.-C, Reed, C A.: J. Am. Chem. Soc 95, 7868 (1973) 104. Collman, J. P., Gagne, R. R., Reed, C A., Halbert, T. R., Lang, G., Robinson, W. T.: ibid. 96, 1427 (1975) 105. Anzui, K., Hatano, K.: Chem. Pharm. Bull. 32, 1273 (1984) 106. Freilag, R. A., Whitten, D. G.: J. Phys. Chem. 87, 3918 (1983) 107. Freilag, R. A., Whitten, D. G.: J. Am. Chem. Soe 103, 1226 (1981) 108. Collman, J. P., Gagne, R. R., Reed, C A., Robinson, W. T., Rodley, G. A.: Proe Natl. Acad. Sci. U.S.A. 71, 1326 (1974) 109. Jameson, G. B., Molinaro. F. S., Ibers, J. A., Collman, J. P., Brauman, J. I., Rose, E., Suslick, K. S.: J. Am. Chem. Soe 102, 3224 (1980) 110. Collman, J. P., Gagne, R. R., Gray, H. B., Hare, J. W.: ibid. 96, 6522 (1974) 111. Collman, J. P., Brauman, J. I., Halbert, T. R., Suslick, K. S.: Proe Natl. Acad. Sci. U.S.A. 73, 3333 (1976) 112. Gmai, H., Nakata, K., Nakatsubo, A., Kakagawa, S.. Vcrmori, Y., Kyuno, E.: Synth. React. Inorg. Met.-Org. Chem. 13, 761 (1983) 113. Baldwin, J. E., Perlmutter, P.: Top. Curr. Chem. 121 (Host Guest Complex Chem. 3), 181 (1984) 114. David, S., Dolphin, D., James. B. R.: in Frontiers of Bioinorganic Chemistry (ed. Xavier, A. V.), VCH Verlagsgesellschaft, Weinheim, pp. 163-182 (1985) 115. Collman, J. P., Gagne. R. R.. Reed, C A.: J. Am. Chem. Soe 96, 2629 (1974) 116. Collman, J. P., Brauman, J. I., Suslick, K. S.: ibid. 97, 7185 (1975) 117. Bogatskii, A. V., Zhilina, Z. I., Danilina, N. I.: Dokl. Akad. Nauk. S.S.S.R. (Engl. Ed.)252, 127 (1980) 118. Bogatskii, A. V., Zhilina, Z. I., Krasnoshchekaya, S. P.. Zakharova, R. M.: Zh. Org. Khim. Engl. Ed. 18, 2035 (1982) 119. Valiotti, A., Adeyemo, A., Williams, F. A., Ricks, L., North, J., Hambright, P.: J. Inorg. Nucl. Chem. 43, 2653 (1981)
202 121. Buckingham, D. H., Clark, C R., Webley, W. S.: J. Chem. Soc Chem. Commun., 192 (1981) 122. Buckingham, D. A., Gunter, M. G.. Mander, L. N.: J. Am. Chem. Soc 100, 2899 (1978) 123. Gunter, M. G., Mander, L. N., McLaughlin, G. M., Murray, K. S.. Berry, K. J., Clark, P. E., Buckingham, D. A.: ibid. 102, 1470 (1980) 124. Elliott. C M.. Krebs, R. R.: ibid. 104, 4301 (1982) 125. Groves, J. T., Myers, R. S.: ibid. 105, 5791 (1983) 126. Tabushi. I., Kodera. M.. Yokoyama, M.: ibid. 107, 4466 (1985) 127. Lecas-Nawrocka. A., Levisalles, J., Mariacher, C, Renko, Z., Rose, E.: Can. J. Chem. 62, 2054 (1984) 128. Collman, J. P., Brauman. J. I., Doxsee, K. M.. Sessler, J. L.. Morris. R. M.. Gibson, O. H.: Inorg. Chem. 22, 1427 (1983) 129. Collman, J. P.. Brauman, J. I., Doxsee, K. M., Halbert, T. R.,Suslick, K. S.: Proc. Natl. Acad. Sci. U.S.A. 75, 564 (1978) 130. Collman, J. P., Brauman, J. I., Doxsee. K. M.: ibid. 76, 6035 (1979) 131. Almog, J., Baldwin, J. E., Dyer, R. L., Peters, M.: J. Am. Chem. Soc 97, 226 (1975) 132. Almog, J.. Baldwin, J. E., Crossley, MK. J., De Bernardis, J. F., Dyer, R. L., Huff, J. R., Peters, M. K.: Tetrahedron 37, 3589 (1981) 133. Ellis, Jr., P. E., Linard, J. E., Szymanski, T., Jones. R. D., Budge, J. R., Basolo, F.: J. Am. Chem. Soc 102, 1889 (1980) 134. Budge, J. R., Ellis, Jr., P. E.Jones, R. D., Linard, J. E., Basolo, F., Baldwin. J. E., Dyer. R. L.: ibid. 101, 4760 (1979) 135. Ellis, Jr., P. E., Linard, J. E., Jones, R. D., Budge, J. R., Basolo, F.: ibid. 102, 1896 (1980) 136. Hashimoto, T., Dyer, R. L., Crossley, M. J., Baldwin. J. E., Basolo, F.: ibid. 104, 2101 (1982) 137. Baldwin, J. E., Crossley, M. G., De Bernardis, J.: Tetrahedron 38, 685 (1982) 138. Shimizu, M., Basolo, F., Vallejo, M. N., Baldwin, J. E.: Inorg. Chim. Acta 91, 247 (1984) 139. Shimizu, M., Basolo, F.. Vallejo, N. M., Baldwin. J. E.: ibid. 91, 251 (1984) 140. Rose, E. J., Vankatasurbramanian, P. N., Swartz, J. C, Jones, R. D., Basolo, F., Hoffman, B. M.: Proc. Natl. Acad. Sci. U.S.A. 79, 5742 (1982) 141. Jameson, G. B., Ibers, J. A.: J. Am. Chem. Soc 102, 2823 (1980) 142. Sabat, M., Ibers, J. A.: ibid. 104, 3715 (1982) 143. Clayden, N. J., Moore, G. R., Williams, R. J. P., Baldwin. J. E., Crossley, M. J.: J. Chem. Soe, Perkin Trans. 2, 1693 (1982) 144. Clayden, N. J., Moore, G. R.. Williams. R. J. P.. Baldwin. J. E., Crossley, M. J.: ibid. 2, 1863 (1983) 145. Baldwin, J. E., Cameron, J. H., Crossley, M. J., Dayley, E. J.: J. Chem. Soe, Dalton Trans., 1739 (1984) 146. Collman, J. P., Brauman, J. I., Collins, T. J., Iverson, B. L., Sessler, J. L.: J. Am. Chem. Soe 103, 2450 (1981) 147. Collman, J. P., Brauman, J. I., Collins, T. J.. Iverson, B. L., Lang. G., Pettman. R. B., Sessler, J. L., Walters. M. A.: ibid. 105, 3038 (1983) 148. Collman, J. P., Brauman. J. I., Iverson, B. L., Sessler, J. L., Morris, R. M.. Gibson, O. H.: ibid. 105, 3052 (1983) 149. Amundsen, A. R., Vaska, L.: Inorg. Chim. Acta. 14, L49 (1975) 150. Suslick, K. S., Fox, M. M.: J. Am. Chem. Soe 105, 3507 (1983) 151. Lindsey, J. S., Mauzerall, D. C: ibid. 104, 4498 (1982) 152. Lindsey, J. S., Mauzerall. D. C, Linschitz, H.: ibid. 105, 6528 (1983) 153. Ogoshi, H., Sugimoto, H.. Yoshida, Z.: Tetrahedron Lett., 4481 (1976) 154. Ogoshi, H., Sugimoto, H.. Yoshida, Z.: ibid. 1515 (1977) 155. Ogoshi, H., Sugimoto, H., Miyake, M., Yoshida, Z. I.: Tetrahedron 40, 579 (1984) 156. Battersby, A. R., Buckley, D. G., Hartley, S. G., Turnbull, M.: J. Chem. Soe, Chem. Commun., 879 (1976) 157. Chang, C. K., Kuo, M.-S.: J. Am. Chem. Soe 101, 3413 (1979) 158. Ward, B., Wang, C-B., Chang, C K.: ibid. 103, 5236 (1981) 159. Yu. N.-T., Kerr, E. A., Ward, B., Chang, C K.: Biochemistry 22, 4534 (1983) 160. Baldwin, J. E.. Klose, T., Peters. M.: J. Chem. Soe, Chem. Commun.. 881 (1976) 161. Baldwin, J. E., Crossley, M. J., Klose. T.. O'Rcar III, E. A., Peters, M. K.: Tetrahedron^, 27 (1981)
203 163. Wijesekera. T. P.: Ph.D. Thesis. University of British Columbia 1980 164. Wijesekera. T. P., Paine III, J. B., Dolphin. D.. Einstein, F. W. B.. Jones, T.: J. Am. Chem. Soc. 105, 6747 (1983) 165. Diekmann, H.. Chang, C K.. Traylor, T. G.: ibid. 93, 4068 (1971) 166. Traylor, T. G.. Campbell. D.. Tsuchiya, S.: ibid. 101, 4748 (1979) 167. Traylor, T. G.. Campbell, D., Tsuchiya, S., Mitchell, M., Stynes, D. V.: ibid. 102, 5939 (1980) 168. Travlor. T. G.. Mitchell. M. J . Tsuchiya. S., Campbell. D. H.. Stynes, D. V., Koga. N.: ibid. 103. 5234 (1981) 169. Travlor. T. G.. Tsuchiva. S.. Campbell. D.. Mitchell. M., Stvncs, D.. Koga. N.: ibid. 107, 604 (1985) 170. Chanii. C K.. DiNeIIo. R. K.. Dolphin. D.: in Inorganic Syntheses (ed. Busch. D. H.). John Wilev & Sons. New York. Vol. XX. 147 (1980) 171. David. S.. Dolphin, D., James. B. R., Paine. J. B. Ill, Wijesekera. T. P.. Einstein. F. W. B.. Jones. T.: Can. J. Chem. 64. 208 (1986) 172. David. S.: Ph.D. Thesis. University of British Columbia 1985 173. Travlor. T. G.. Koga. N.. Dearduff. L. A.. Swepston, P. N., bers. J. A.: J. Am. Chem. Soc 106, 5132 (1984) 174. Travlor. T. G.. Koga. N.. Dearduff. L. A.: ibid. 107. 6504 (1985) 175. Morgan. B.: Ph.D. Thesis. University of British Columbia 1984 176. Morgan, B., Dolphin, D.: Angew. Chem. Int. Ed. 24, 1003 (1985) 177. Battersby, A. R., Hartley. S. G., Turnbull, M. D.: Tetrahedron Lett., 3169 (1978) 178. Cruse, W. B., Kennard. O., Sheldrick, G. M., Hamilton. A. D., Hartley. S. G., Battersby, A. R.: J. Chem. Soc, Chem. Commun., 700 (1980) 179. Battersby, A. R., Howson, W., Hamilton, A. D.: ibid. 1266 (1982) 180. Chang. C K.: J. Am. Chem. Soc. 99, 2819 (1977) 181. Richardson, N. M., Sutherland, I. O.. Camilleri. P., Page, J. A.: Ictrahedron Lett. 26, 3739 (1985) 182. Bogatskii, A. V.. Zhilina, Z. I., Stepanov, D. E.: Zh. Org. Khim. Engl. Ed. 18, 2039 (1982) 183. Hamilton, A. D., Lehn, J.-M., Sessler, J. L.: J. Chem. Soc., Chem. Commun., 311 (1984) 184. Chang. C K., Koo, M. S., Ward, B.: ibid. 716 (1982) 185. Guntcr. M. J.. Mander, L. N.: J. Org. Chem. 46, 4792 (1981) 186. Gunter, M. J., Mander, L. N., Murray. K. S., Clark, P. E.: J. Am. Chem. Soc. 103, 6784 (1981) 187. Ganesh, K. N., Sanders, J. K. N.: J. Chem. Soc, Chem. Commun., 1129 (1980) 188. Ganesh, K. N.. Sanders, J. K. N.: J. Chem. Soc, Perkin Trans. 1, 1611 (1982) 189. Ganesh. K. N.. Sanders. J. K. N.. Waterton. J. C: ibid. 1. 1617 (1982) 190. Sanders. J. K., Leighton, P.: J. Chem. Soc, Chem. Commun., 24 (1985) 191. Leighton, P., Sanders, J. K. M.: ibid. 854 (1984) 192. Abraham. R. J., Leighton, P., Sanders. J. K. M.: J. Am. Chem. Soc 107, 3472 (1985) 193. Leighton, P.. Sanders. J. K. M.: J. Chem. Soc. Chem. Commun.. 856 (1984) 194. Hamilton. A. D.. Rubin, H.-D.. Bocarsly. A. B.: J. Am. Chem. Soc 106, 7255 (1984) 195. Momenteau. M.. Mispclter. J., Loock. B.. Bisagni. E.: J. Chem. Soc. Perkin Trans. 1, 189 (1983) 196. Momenteau. M.. Loock, B.. Mispelter, J.. Bisagni, E.: Nouv. J. Chem. 3, 77 (1979) 197. Lexa, D., Momcnteau. M., Rentien, P., Rytz, G., Saveant, J. M.. Xu. F.: J. Am. Chem. Soc 106, 4755 (1984) 198. Becker. J. Y.. Dolphin, D., Paine. J. B. III. Wijeskera, T. P.: J. Electroanal. Chem. 164, 335 (1984) 199. Zhilina. Z. I., Bogatskii, A. V.. Vodzinskii, S. V., Abramovich, A. E.: Zh. Org. Khim. Eng. Ed. 18, 227 \ (1982) 200. Wciser, J., Staab, H. A.: Angew. Chem. Int. Ed. 23, 623 (1984) 201. Momenteau, M.. Lavalette D.: J. Chem. Soc, Chem. Commun., 341 (1982) 202. Mispelter. J.. Momcnteau, M., Lavalette, D. Lhoste. J.-M.: J. Am. Chem. Soc 105, 5165 (1983) 203. Momcnteau, M., Loock, B.. Lavalette, D.. Tetreau, C1 Mispelter, J.: J. Chem. Soc, Chem. Commun., 962 (1983) 204. Battersby, A. R., Hamilton, A. D.: ibid. 117 (1980) 205. Battersby, A. R., Bartholomew. S. A. J., Nitta. J.: ibid. 1291 (1983)

Synthesis and Structure of Biomimetic Porphyrins: Brian Morgan and David Dolphin

Uploaded by

Copyright:

Available Formats

Synthesis and Structure of Biomimetic Porphyrins: Brian Morgan and David Dolphin

Uploaded by

Document Information

Original Title

Copyright

Available Formats

Share this document

Share or Embed Document

Sharing Options

Did you find this document useful?

Is this content inappropriate?

Copyright:

Available Formats

Synthesis and Structure of Biomimetic Porphyrins: Brian Morgan and David Dolphin

Uploaded by

Copyright:

Available Formats

Synthesis and Structure of Biomimetic Porphyrins

1. 2. 3. 3. A. 3.B. 3.C. 3. D. 4. 4. A. 4. B. 5. 5. A. 5.B. 5. C 6. 6.A. 6.B. 6.C. 6. D. 7. 8.

functions, for and P450)5. IX), and the of oxygen b,

responsible utilization (cytochrome

(hemoglobin (cytochrome and case ring

hydrogen porphyrin essentially be

peroxide oxidation (usually planar

destruction The the nature nitrogens metal. of the of the a (spin

catalases) ', contains occupying of of be fully be

protoporphyrin coordination by the the of number

diversity tenet may to

Obviously porphyrins state

must and much

characteristics steric and has

electronic focussed which

effects on upon his the

Therefore, the oxygen is irreversible porphyrins must being globin

polypeptide the close

proteins rings fact

sheath iron(II) body hemocomplex

preventing ano her

[-peroxo reduce to ferric

irreversible the (the oxidized

oxidation iron(III) Even 3%. This of for

mechanism the form acid to with

provide incapable exists is

enzyme oxygen body and occurs in is

methemoglobin to or the The the under

hemoglobin alternative protonated the the cytoFe11-O2

transport) the aqueous believed occur

form12. about where

oxidation formation chromes species by

inhibited, Similar and

assisted of chain also

oxyhemoglobin terminal backbone changes the oxygen is upon

oxymyoglobin and the

due distal a are to is

imidazole than at has simply the been iron the i.e., In by

remarkable residues transfer

cooperativity occur sphere iron

exhibited the the is

hemoglobin17. postulated But it

certain electron the

protein's The second for Eq. 9,

coordination simple in over

porphyrin preference for the at of

constants The of one to

Fe11(TPP) porphyrin high spin (S spin =

have is (S 0) for the

four-coordinate ligand form

stabilization fur her iron the iron

contrast, this by self is an

coordinated makes control have

six-coordinate Im-Fe-SR2, range in of

concentration of five-coordinate heme and reduce u-peroxo complex formation.

Temperatures22-'25. where to the reduced studying

complexes reactions as binding

are are K2/K1

(iii) ible Ior